CA1338235C - Esters of alginic acid - Google Patents

Esters of alginic acid

Info

Publication number
CA1338235C
CA1338235C CA000540467A CA540467A CA1338235C CA 1338235 C CA1338235 C CA 1338235C CA 000540467 A CA000540467 A CA 000540467A CA 540467 A CA540467 A CA 540467A CA 1338235 C CA1338235 C CA 1338235C
Authority
CA
Canada
Prior art keywords
alcohol
ester
alginic acid
surgical
sanitary
Prior art date
Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
Expired - Fee Related
Application number
CA000540467A
Other languages
French (fr)
Inventor
Francesco Della Valle
Aurelio Romeo
Current Assignee (The listed assignees may be inaccurate. Google has not performed a legal analysis and makes no representation or warranty as to the accuracy of the list.)
Fidia SpA
Original Assignee
Fidia SpA
Priority date (The priority date is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the date listed.)
Filing date
Publication date
Application filed by Fidia SpA filed Critical Fidia SpA
Priority to CA000616909A priority Critical patent/CA1338236C/en
Application granted granted Critical
Publication of CA1338235C publication Critical patent/CA1338235C/en
Anticipated expiration legal-status Critical
Expired - Fee Related legal-status Critical Current

Links

Classifications

    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/0012Galenical forms characterised by the site of application
    • A61K9/0014Skin, i.e. galenical aspects of topical compositions
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K47/00Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient
    • A61K47/30Macromolecular organic or inorganic compounds, e.g. inorganic polyphosphates
    • A61K47/36Polysaccharides; Derivatives thereof, e.g. gums, starch, alginate, dextrin, hyaluronic acid, chitosan, inulin, agar or pectin
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K47/00Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient
    • A61K47/50Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient the non-active ingredient being chemically bound to the active ingredient, e.g. polymer-drug conjugates
    • A61K47/51Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient the non-active ingredient being chemically bound to the active ingredient, e.g. polymer-drug conjugates the non-active ingredient being a modifying agent
    • A61K47/56Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient the non-active ingredient being chemically bound to the active ingredient, e.g. polymer-drug conjugates the non-active ingredient being a modifying agent the modifying agent being an organic macromolecular compound, e.g. an oligomeric, polymeric or dendrimeric molecule
    • A61K47/61Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient the non-active ingredient being chemically bound to the active ingredient, e.g. polymer-drug conjugates the non-active ingredient being a modifying agent the modifying agent being an organic macromolecular compound, e.g. an oligomeric, polymeric or dendrimeric molecule the organic macromolecular compound being a polysaccharide or a derivative thereof
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K8/00Cosmetics or similar toiletry preparations
    • A61K8/18Cosmetics or similar toiletry preparations characterised by the composition
    • A61K8/72Cosmetics or similar toiletry preparations characterised by the composition containing organic macromolecular compounds
    • A61K8/73Polysaccharides
    • A61K8/733Alginic acid; Salts thereof
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K9/00Medicinal preparations characterised by special physical form
    • A61K9/0012Galenical forms characterised by the site of application
    • A61K9/0019Injectable compositions; Intramuscular, intravenous, arterial, subcutaneous administration; Compositions to be administered through the skin in an invasive manner
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61LMETHODS OR APPARATUS FOR STERILISING MATERIALS OR OBJECTS IN GENERAL; DISINFECTION, STERILISATION OR DEODORISATION OF AIR; CHEMICAL ASPECTS OF BANDAGES, DRESSINGS, ABSORBENT PADS OR SURGICAL ARTICLES; MATERIALS FOR BANDAGES, DRESSINGS, ABSORBENT PADS OR SURGICAL ARTICLES
    • A61L15/00Chemical aspects of, or use of materials for, bandages, dressings or absorbent pads
    • A61L15/16Bandages, dressings or absorbent pads for physiological fluids such as urine or blood, e.g. sanitary towels, tampons
    • A61L15/22Bandages, dressings or absorbent pads for physiological fluids such as urine or blood, e.g. sanitary towels, tampons containing macromolecular materials
    • A61L15/28Polysaccharides or their derivatives
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61LMETHODS OR APPARATUS FOR STERILISING MATERIALS OR OBJECTS IN GENERAL; DISINFECTION, STERILISATION OR DEODORISATION OF AIR; CHEMICAL ASPECTS OF BANDAGES, DRESSINGS, ABSORBENT PADS OR SURGICAL ARTICLES; MATERIALS FOR BANDAGES, DRESSINGS, ABSORBENT PADS OR SURGICAL ARTICLES
    • A61L17/00Materials for surgical sutures or for ligaturing blood vessels ; Materials for prostheses or catheters
    • A61L17/06At least partially resorbable materials
    • A61L17/10At least partially resorbable materials containing macromolecular materials
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61LMETHODS OR APPARATUS FOR STERILISING MATERIALS OR OBJECTS IN GENERAL; DISINFECTION, STERILISATION OR DEODORISATION OF AIR; CHEMICAL ASPECTS OF BANDAGES, DRESSINGS, ABSORBENT PADS OR SURGICAL ARTICLES; MATERIALS FOR BANDAGES, DRESSINGS, ABSORBENT PADS OR SURGICAL ARTICLES
    • A61L27/00Materials for grafts or prostheses or for coating grafts or prostheses
    • A61L27/14Macromolecular materials
    • A61L27/20Polysaccharides
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61QSPECIFIC USE OF COSMETICS OR SIMILAR TOILETRY PREPARATIONS
    • A61Q19/00Preparations for care of the skin
    • CCHEMISTRY; METALLURGY
    • C08ORGANIC MACROMOLECULAR COMPOUNDS; THEIR PREPARATION OR CHEMICAL WORKING-UP; COMPOSITIONS BASED THEREON
    • C08BPOLYSACCHARIDES; DERIVATIVES THEREOF
    • C08B37/00Preparation of polysaccharides not provided for in groups C08B1/00 - C08B35/00; Derivatives thereof
    • C08B37/006Heteroglycans, i.e. polysaccharides having more than one sugar residue in the main chain in either alternating or less regular sequence; Gellans; Succinoglycans; Arabinogalactans; Tragacanth or gum tragacanth or traganth from Astragalus; Gum Karaya from Sterculia urens; Gum Ghatti from Anogeissus latifolia; Derivatives thereof
    • C08B37/0084Guluromannuronans, e.g. alginic acid, i.e. D-mannuronic acid and D-guluronic acid units linked with alternating alpha- and beta-1,4-glycosidic bonds; Derivatives thereof, e.g. alginates

Landscapes

  • Health & Medical Sciences (AREA)
  • Life Sciences & Earth Sciences (AREA)
  • Chemical & Material Sciences (AREA)
  • General Health & Medical Sciences (AREA)
  • Public Health (AREA)
  • Animal Behavior & Ethology (AREA)
  • Veterinary Medicine (AREA)
  • Epidemiology (AREA)
  • Medicinal Chemistry (AREA)
  • Engineering & Computer Science (AREA)
  • Dermatology (AREA)
  • Pharmacology & Pharmacy (AREA)
  • Materials Engineering (AREA)
  • Molecular Biology (AREA)
  • Birds (AREA)
  • Surgery (AREA)
  • Oral & Maxillofacial Surgery (AREA)
  • Transplantation (AREA)
  • Hematology (AREA)
  • Biochemistry (AREA)
  • Chemical Kinetics & Catalysis (AREA)
  • Polymers & Plastics (AREA)
  • Organic Chemistry (AREA)
  • Bioinformatics & Cheminformatics (AREA)
  • Vascular Medicine (AREA)
  • Inorganic Chemistry (AREA)
  • Medicinal Preparation (AREA)
  • Polysaccharides And Polysaccharide Derivatives (AREA)
  • Cosmetics (AREA)
  • Materials For Medical Uses (AREA)
  • Pharmaceuticals Containing Other Organic And Inorganic Compounds (AREA)
  • Detergent Compositions (AREA)
  • General Preparation And Processing Of Foods (AREA)
  • Jellies, Jams, And Syrups (AREA)
  • Plural Heterocyclic Compounds (AREA)
  • Manufacture Of Macromolecular Shaped Articles (AREA)

Abstract

Sanitary or surgical articles are provided, the essential component of which comprises at least one total, water-insoluble ester of alginic acid with an alcohol. In such esters, the alcohol is selected from the group consisting of aliphatic, araliphatic, cycloaliphatic, aliphatic-cycloaliphatic and heterocyclic alcohols. These esters may be used as sanitary or surgical articles because they possess interesting and valuable bioplastic and pharmaceutical qualities.

Description

This invention relates to sanitary or surgical articles comprising at least one total, water-insoluble ester of alginic acid with an alcohol, and to processes for the preparation thereof and procedures for the uses thereof.
Alginic acid is a natural acidic polysaccharide extracted above all from so-called brown algae G

(PhaecoPhYceae) with a high molecular weight varying between 30,000 and 200,000, and containing chains formed by D-mannuronic acid and L-guluronic acid. The degree of polymerization varies according to the type of alga used for extraction, the season in which the algae were gathered and the place of origin of the algae, as well as the age of the plant itself. The main species of brown algae used to obtain alginic acid are, for e~ample, MacrocYstis PYrifera, Laminaria cloustoni, Laminaria hYPerborea, Laminaria fle~icaulis. Laminaria diqitata, AscoPhYllum nodosum, Fucus serratus.
Alginic acid is found in these algae as an e~ten-sive constituent of the cell walls in the form of a mixture of some of its alkaline salts, of these especially sodium salt. This mi~ture is also known as ~algin~. These salts are normally e~tracted in aqueous conditions with a sodium carbonate solution and it is possible to obtain alginic acid directly from this extract by precipitation with an acid, for e~ample a mineral acid e.g. hydrochloric acid. An indirect preparation procedure involves first making an insoluble calcium salt by adding a soluble calcium salt, e.g.
chloride, and after washing this salt, alginic acid is obtained again by treatment with an acid.
Alginic acid or alkaline alginates may, however, also be obtained microbiologically, for instance by fermentation with Pseudomonas aeruqinosa or mutants of Pseudomonas putida, Pseudomonas fluorescens or Pseudomonas mendocina.

.'~

. _ 3 _ 1 3 3 8 2 3 5 The metal salts of alginic acid, especially the alkaline and alkaline earth metal salts, have in-teresting chemical and physical properties and are therefore widely used in industry, Thus, for e~ample, the solutions of alkaline or alkaline earth alginates are extremely suitable, due to their viscosity, and their adjustability by temperature and pH, for the preparation of gels which may be widely used in the food industry, for the preparation of ice creams, milk puddings and many other types of cakes and puddings.
Another property which is widely e~ploited in the field of alimentation is the ability of alginates to retain water, and for this reason they are used for e~ample for the conservation of many types of frozen foods. A third property of alginates is their power to emulsify and to stabilise emulsions; for this reason too these salts are important in the food industry, where they are used for the preparation of condiments and for the stabilisation of many types of drink, e.g. beer or fruit juices, sauces and syrups.
The ability of alginate solutions to form films and fibres has been exploited in the paper industry, in making adhesive labels, in textile printing and dyeing, and in the preparation of sanitary, medical and surgical articles. Alginates are used as emulsifiers for the preparation of polishes, antifoam agents, lactics and as stabilisers in the ceramic and detergent industries (for a more detailed list see for example ~The Polysaccharides~, Vol. 2, by Paul A. Sandford and John Baird, Copyright 1983 by Academic Press., Inc.).

- ~' 1 33823~

Alginic acid and its salts have also been used however in the pharmaceutical, medical, surgical and cosmetic fields, for e2ample for the preparation of medicaments for topical use and sanitary and surgical articles. For example the German Offenlegungsschrift 3 017 221 (20.11.1980), discloses an "artificial skin~ for use in serious lesions of the skin, for e~ample following burns, in which an ointment containing a soluble alginate of an alkaline metal is applied topically to the skin and treated in situ with a soluble calcium salt. This causes the formation of insoluble calcium alginate, transforming the layer of ointment into an easily tolerated biologically protective film, with structural and mechanical physical characteri-stics similar to those of natural skin.
Calcium alginate has been used for the manufacture of fibres for use in the pharmaceutical industry French patent application No. 2 418 821 (28.9.1979), Rumanian patent No.70 069 (30.6.1980) contains the description of a healing and antiseptic medicament for skin wounds, made from calcium alginate fibres. Calcium alginate is also used as a hemostatic agent in the form of bandages or gauzes. containing fibres of the salt. Other medicaments based on calcium alginate are used for the treatment of sinoids, fistulas, and;in the treatment of nosebleeds. In Galenism, sodium and calcium alginates are also used as disintegrators for pills, and sodium alginate is also used for its binding properties.
Also used in industry in many of the abovementioned fields are two alginic acid- esters or salts of such ` -esters, more precisely ethylene glycol and propylene glycol esters. The latter is used for e~ample as an emulsifier and stabiliser for foodstuffs. (See for example "Martindale" - The E~-tra Pharmacopoeia, p. 931 and ~The Polysaccharides", Vol. 2, Copyright by Academic Press, Inc. 1983, pp. 448-449). The above mentioned esters have been obtained by reaction of alginic acid, or its salt or partial salt, with ethylene or propylene o~ide respectively. This preparation process is also the basis of patents for the preparation of the above mentioned alginic acid esters and esters of bivalent alcohols by reaction of an aliphatic hydrocarbon epo~ide, possibly substituted or interrupted by hetero atoms in the carbon atom chain (see for example U.S.
Patent Nos. 2,463,824 - 2,426,125 - 2,463,824, German Offenlegungsschriften 2,161,415 - 2,046,966 - 2,641,303 - 2,529,086, Japanese Patent Nos. 2027 ('59) and 72 47 858, and French Patent No. 2247204.
The alginic acid esters obtainable by the action of the above mentioned epoxides on the free acid or its salts are partial esters (see A.B. Steiner, Industrial and Engineering Chemistry, Vol.43, pp. 2073 - 2077, 1951), with a ma~imum degree of esterification of 80% of all the existing carboxylic groups in the case of glycol esters with a low molecular weight, and a very low degree in the case o glycol esters with long chains. It has not been possible until now to prepare total esters by this process.
Monovalent alcohol esters, both aliphatic and araliphatic have also been mentioned in literature, above all a methyl ester of alginic acid obtained by reaction of alginic acid in an ethereal solution of diazomethane. (Zeitschrift fuer physiologische Chemie, Vol. 293, p. 121, 1953, A.B. Steiner, Industrial and ~ngineering Chemistry, Vol. 43, p. 2073, 1951, U.K.
Patent No. 768,309. It seems however that the products obtained by reaction with diazomethane are not really alginic acid esters but rather methyl esters of an alginic acid partially etherified to the hydro~y alcohol groups, as described for e~ample in E~ample 4 of the above mentioned U.K. patent. One methyl ester has also been obtained by reaction of dimethyl sulphate on a soluble salt of alginic acid in an organic solvent with low solubility in water, but in the presence of water (U.S. Patent No. 2,860,130). The product obtained, referred to as methyl alginic acid or methyl alginate, is not to be considered as a pure ester, since it is known that sugar hydro~yls are easily etherified with this methylating agent. This case, therefore, also is truly a mi~ed ester-ether.
Also mentioned in literature are alginic acid esters of monovalent alcohols, with no indication however of their preparation process and no description of their chemical and physical properties. As no preparation process is known, apart from the above mentioned reaction with diazomethane and dimethyl sulphate, it is probable that the use of homologues of these esterifying agents to obtain esters of tAe homologous series of the methyl ester are not practical at all, or at the most they result in mi~ed products, as in the case of methyl ~A~
.
`.L~.

` 7 l 33823~
products. (See for example U.S. Patent No. 4,216,104 in which a propyl alginate is mentioned with no indication of its origin or preparation process, and the Japanese Kokai No. 55-132781, page 5, in which ethyl, butyl, lauryl, oleyl, phenyl and benzyl esters are mentioned, with no indication as to how they are obtained.
on the basis of these facts therefore, it is presumed that, of all alginic acid esters, only those esters of bivalent alcohols are known, and more precisely, only the partial esters with glycols. By the known process used in industry, it is difficult to achieve complete esterification. In the commercial product, no less than 10~ of the carboxyls remain unesterified in their free carboxy form, possibly salified.
An object of a principal aspect of this invention is therefore to provide novel uses of novel alginic acid esters (or alginic esters) in medicine and surgery.
An object of another aspect of this invention is to provide articles containing total, water-insoluble esters of alginic acid for use in biodegradable plastic materials for medical-surgical use.
By one broad aspect of this invention, sanitary or surgical articles are provided, the essential component of which is at least one total, water-insoluble ester of alginic acid with an alcohol which is selected from the group consisting of aliphatic, araliphatic, cycloaliphatic, aliphatic-cycloaliphatic and heterocyclic alcohols.

G

_ 8 These articles containing such compounds possess interesting and valuable bioplastic qualities, so that they may be used in numerous fields, e.g. in surgery and medicine.
By one variant thereof, in the alginic acid total, water-insoluble esters, the alcohol may include: (a) an aliphatic radical with a maximum of 34 carbon atoms; (b) an araliphatic radical with only one benzene ring, and in which the aliphatic chain has a minimum of 4 carbon atoms;
(c) a cycloaliphatic radical which is monocyclic or polycyclic with a maximum of 34 carbon atoms; (d) an aliphatic-cycloaliphatic radical which is monocyclic or polycyclic with a maximum of 34 carbon atoms; or (e) a heterocyclic radical with a maximum of 34 carbon atoms in which the hetero atoms are selected from the group consisting of oxygen, sulfur and nitrogen. In a variation of such variant, a) the aliphatic, cycloaliphatic, alipha-tic-cycloaliphatic or heterocyclic radicals may be substi-tuted by one or two functional groups selected from the group consisting of amino, hydroxy, mercapto, aldehydo, keto, carboxyl, hydrocarbyl, dihydrocarbylamino, ether, ester, thioether, thioester, acetal, ketal, carbal-koxy and carbamidic groups and carbamidic groups substi-tuted by one or two alkyl groups, the hydrocarbyl radicals in these functional groups having a maximum of 6 carbon atoms; or b) the araliphatic radicals may be substituted in the benzene residue with 1-3 substituents selected from the group consisting of methyl, hydroxy and halogen, or may be G

g substituted in the aliphatic portion with one or two functional groups selected from the group consisting of methyl, ethyl, diethyl, pyrrolidine and piperidine groups.
By still another variation of such variant, a) the hydro-carbyl radicals of the functional groups are Cl~4 alkylgroups; b) the amino or substituted carbamidic groups are C18 alkylene amine or Cl8 alkylene carbamidic groups; or c) the cycloaliphatic, aliphatic-cycloaliphatic or hetero-cyclic moieties are monocyclic with a maximum of 12 carbon atoms and the ring has between 5 and 7 carbon atoms.
By another variant thereof, the aliphatic radical may be derived from a member selected from the group consisting of methyl alcohol, ethyl alcohol, propyl alcohol, isopropyl alcohol, n-butyl alcohol, isobutyl alcohol, tert-butyl alcohol, amyl alcohol, pentyl alcohol, hexyl alcohol, octyl alcohol, glycerin, tartronic alcohol, lactic acids, gly-colic acid, malic acid, tartaric acid, citric acid, amino-ethanol, aminopropanol, n-aminobutanol or their dimethyl or diethyl derivatives in the amino moiety, choline, pyrroli-dinylethanol, piperidinylethanol, piperazinylethanol,piperazinyl-n-propyl alcohol, piperazinyl-n-butyl alcohol, monothioethylene glycol, myricyl alcohol, citronellol, geraniol, nerol, nerolidol, linalool, farnesol and phytol.
Preferred total, water-insoluble esters of alginic acid include the total, water-insoluble methyl ester of alginic acid; the total, water-insoluble ethyl of alginic acid; the total, water-insoluble tert-butyl ester of alginic acid; and the total, water-insoluble benzyl ester of alginic acid.
The above-described sanitary or surgical articles may be in the form of a film or thread.
By yet another aspect of this invention, a procedure is provided for the preparation of sanitary or surgical articles in the form of films or threads of at least one total, water-insoluble ester of alginic acid with an alcohol selected from the group consisting of aliphatic, araliphatic, cycloaliphatic, aliphatic-cycloaliphatic and heterocyclic alcohols, the procedure comprising: dissolving the total, water-insoluble alginic ester in a first organic solvent; making the solution into sheet form or thread form, respectively; then eliminating the first organic solvent by treatment with a second suitable organic solvent or with an aqueous solvent which is soluble in the first solvent; and then removing the second organic or aqueous solvent.
In the above procedure, the alcohol may be one or a mixture of the alcohols previously disclosed hereinabove.
The invention claimed in a divisional application based on the present application, and also taught in the present specification relates to a simple and very convenient procedure for the preparation of total, water-insoluble alginic esters, based on the treatment of quater-nary ammonium salts of alginic acid with conventional alkylating agents in organic, preferably aprotic, solvents, e.g., in dimethylsulfoxide, making a large number of new total, water-insoluble alginic esters available, especially those esters of monovalent alcohols, e.g., homologues of methyl ester, and esters of aromatic, araliphatic, alicyclic and heterocyclic alcohols. The new procedure may be used also for the preparation of total, water-insoluble esters deriving from substituted alcohols, in particular known esters of bivalent aliphatic alcohols, obtainable by the reaction of alginic acid with liphatic epoxides, as described above, and mainly new total, water-insoluble esters of such bivalent alcohols.
The new total, water-insoluble alginic esters, claimed in the above-referred-to divisional application, may be used according to aspects of the present invention, in the sanitary and surgical fields, where metal alginates or the esters of aliphatic bivalent alcohols of the type of pro-pylene glycol esters of alginic acid have already been used. Therefore, the present invention in one of its aspects is represented by both this use of the new total, water-insoluble esters, and the corresponding articles and industrial products, e.g. sanitary and surgical articles.
With the discovery of the new total, water-insoluble alginic esters as claimed in the a~ove-referred-to divisional application, a new use of alginic esters in general has also been provided in that divisional application, that is, for the new total, water-insoluble esters and for those already known. This new use is their use as vehicles for pharmaceutically-active substances, especially those with a topical, oral or rectal action, but also those for parenteral administration, as provided in a divisional application of the present application. The use of known alginic esters of bivalent alcohols was previously limited to the function of emulsifying agents, emulsion stabilisers, thickening agents and possibly related uses.
No use in the pharmaceutical, sanitary, medical, surgical or cosmetic fields was envisaged for those esters. The invention provided by the heretofore-mentioned divisional application therefore concerns the above-mentioned use and respective products, especially, the pharmaceutical preparations containing an total, water-insoluble alginic ester as vehicle for the active substances.
In such pharmaceutical preparations, the active sub-stance may also be vehicled by the new total, water-insoluble esters which have a pharmacologically-active substance as their alcohol component. Of the pharma-ceutical preparations provided by the heretofore-mentioned divisional application, therefore, particularly interesting are those containing an total, water-insoluble alginic ester deriving from a therapeutically-active alcohol, e.g., those mentioned hereafter, that is, total, water-insoluble esters comprised of alginic acid esterif ied with the alcohol moiety of a therapeutically-active compound.
The use of the above-mentioned alkaline alginates of the prior art in the various sectors of industry, pharma-ceutics, surgery and above all in the food industry, presented some disadvantages when they were used in acid G

conditions, because of the resulting release of alginic acid with low solubility which may separate in the solid state. Also in the presence of calcium ions, some insol-uble products containing calcium alginate may separate, and for this reason alkaline alginates have been unsuitable for use in liquids containing the above-mentioned ions, for example, in products containing milk or milk derivatives.
For this reason the above-mentioned soluble salts of alginic acid have, in the past, been substituted by the above-mentioned glycol esters, especially propylene glycol ester, in those cases in which it was essential to maintain a good level of solubility in acid conditions, or in the presence of calcium salts, e.g., when the alginate was used as emulsifier or emulsion stabiliser. The glycol esters of alginic acid are however toxic to a certain extent and their use must be limited. This is due to the intrinsic toxicity of the glycol residue, the part which is absorbed and metabolised.
The invention provided by the heretofore-mentioned divisional application makes available to the above-mentioned various industrial and scientific fields an assortment of new products with properties essentially similar to those of alkaline alginates or the already known glycol esters, but with effects which are more in keeping with the requirements of increasingly perfected products, and these effects naturally vary from case to case according to the use to which the new products are put. It is important to underscore, first and foremost, the superiority of the monovalent total, water-insoluble esters according to the invention provided by the heretofore-mentioned divisional application over the above-known glycol esters, since the monovalent alcohol residues are metabolised in the organism to degraded products which are less toxic than the glycols. This is naturally true of total, water-insoluble esters deriving from alcohols which do not contain toxic substitutes, especially aliphatic, cycloaliphatic, monovalent alcohols. These new total, water-insoluble esters will be of great advantage above all in sanitary or surgical articles, as provided herein by the present invention.
The low level of toxicity of the total, water-insoluble esters of numerous monovalent alcohols of alginic acid according to the invention provided by the heretofore-mentioned divisional application may be exploited in the pharmaceutical, cosmetic and sanitary-surgical fields, where the new total, water-insoluble alginic esters may be used as biodegradable plastic materials with various functions as the case may be. Thus, for example, the total, water-insoluble alginic esters may be used as additives for the wide range of polymeric materials used for sanitary and surgical articles according to the present invention, e.g., polyurethanes, polyesters, polyolefins, polyamides, polysiloxanes, vinyl and acrylic polymers, with the effect of rendering these materials biocompatible.
In this case, the addition of a total, water-insoluble G

alginic ester is carried out, for example, by coating the surface of these materials or by dispersion in the same or by a combination of both procedures. These materials may be used for the manufacture of various sanitary and medical articles e.g. cardiac valves, intraocular lenses, vascular clips, pace-makers and the like, including these types of articles discussed in U.S. Patent No. 4,500,676.
In the cosmetic and pharmaceutical fields, the total, water-insoluble alginic esters of the invention provided by the heretofore-mentioned divisional application may be used for the preparation of ointments, creams and other types of medicaments for topical application or cosmetic products, e.g., sunshield creams, where they act as stabilisers and emulsifiers having a greater degree of stability than the alkaline alginates of the prior art, especially with regard to higher temperatures, and a lesser degree of toxicity compared to glycol esters. In pharmaceuticals, they may be used to the same advantage as disintegrators for pills or as a binding agent, but above all, according to a parti-cularly important aspect of the invention provided by theheretofore-mentioned divisional application, as a vehicle for pharmacologically-active substances, especially those for topical use. This vehicling action of the new total, water-insoluble esters may be carried out various ways, specifically including: 1) the total, water-insoluble alginic ester serves as vehicle and is associated mechanically, physically mixed with the active substance;
and 2) the total, water-insoluble alginic ester is G

1 33823~

esterified with an alcohol which represents the active substance.
Apart from these two variations, combinations of the same may be used, for example, a combination (1) and (2).
In the case of variation (2), it is possible to vary and combine the alcohol residues in the total, water-insoluble alginic ester, and it is possible to have total, water-insoluble esters of a mixed character, in which the alcohol residues derive partly from pharmacologically-inactive alcohols and partly from pharmacologically-active alcohols.
It is possible to have, in the same total, water-insoluble ester, both inactive alcohol residues and residues of therapeutically-active alcohols.
A first group of total, water-insoluble esters useful according to the present invention, suitable for use in the above-mentioned industrial sectors, e.g. in the preparation of sanitary, medical and surgical articles, etc., is represented by those total, water-insoluble esters in which the properties of the alginic component are the properties to be exploited. These total, water-insoluble esters derive from alcohols of the aliphatic, aromatic, arali-phatic, cycloaliphatic or heterocyclic series which have no toxic or pharmacological action, e.g. for example the saturated alcohols of the aliphatic series or simple alcohols of the cycloaliphatic series. Examples of these alcohols are mentioned hereinafter.
A second group of total, water-insoluble esters for use in therapy in the invention provided by the heretofore-G

17mentioned divisional application is represented by the total, water-insoluble esters in which the pharmacological qualities of the alcohol component are dominant, that is, total, water-insoluble alginic acid esters with pharmaco-logically-active alcohols, e.g., steroidal alcohols, e.g., those of the cortisone type. These total, water-insoluble esters possess properties which are qualitatively similar to those of the alcohol, but with a wider range of action.
Even as compared to already known esters of such pharmaceutically-active alcohols, the total, water-insoluble alginic esters ensure a more balanced constant and regular pharmacological action and generally cause a marked retard effect of the active alcohol component.
A third group of total, water-insoluble alginic acid esters according to the invention provided by the heretofore-mentioned divisional application, and representing a particularly original and useful aspect of the same, is that of the total, water-insoluble esters of a more mixed character compared to the two previous groups.
That is, total, water-insoluble esters in which part of the carboxylic groups of alginic acid are esterified with a pharmacologically-inactive alcohol, or the activity of which is negligible. By suitably dosing the percentages of the two types of alcohols as the esterifying component, it is possible to obtain total, water-insoluble esters with the same activity as the pharmacologically-active alcohol and having those qualities mentioned above increased stability and bioavailability compared to the desired and characteristic activity of the pharmacologically-active alcohol and due to the ester groups of the pharma-cologically-inert alcohol.
A fourth group of total, water-insoluble esters provided by the heretofore-mentioned divisional application is represented by those of a mixed character in which the ester groups derive from two different therapeutically-active substances. In this case also, the total, water-insoluble esters are total, that is, all of the carboxylic groups derive from two different therapeutically-active alcohols, for example, from a cortisone steroid and from an antibiotic. It is possible, however, to prepare total, water-insoluble esters with three or more alcoholic components, for example, total, water-insoluble esters in which a part of the carboxylic groups is esterified with a therapeutically-active alcohol, and another port of which is esterified with a therapeutically-inactive alcohol.
Most of the total, water-insoluble esters of alginic acid, in contrast to its salts, present a certain degree of solubility in organic solvents. This solubility depends on the percentage of esterified carboxylic groups and of the type of alkyl group bound to the carboxyl. For example, a total, water-insoluble ester of alginic acid thus obtained presents good solubility at room temperature, for example, in dimethylsulfoxide. The total, water-insoluble esters which are all new are a particular aspect of the invention provided by the heretofore-mentioned divisional application present, on the other hand, poor solubility in water.

19 l 33823~
Thus, for example, the total, water-insoluble esters of monovalent alcohols, e.g. lower and higher alkyl esters, are not very soluble or are insoluble in water and aqueous solutions but also the new total, water-insoluble esters of bivalent alcohols, e.g. the total, water-insoluble ester of the glycols, e.g. ethylene glycol, isobutylene glycol also have such solubility characteristics.
These solubility characteristics, together with the marked viscoelastic properties of total, water-insoluble esters, make them suitable for use in the manufacture of sanitary and medical articles according to the present invention, which are insoluble in saline and have the particular desired form. Such articles may be prepared, for example, by dissolving a total, water-insoluble ester of alginic acid in a first organic solvent, giving the extremely viscous solution the form of the desired article and lastly by extracting the organic solvent with a second solvent which can be mixed with the first, but in which the total, water-insoluble alginic acid ester is insoluble, for example, an alcohol, or water.
The present invention includes the industrial use of the new total, water-insoluble alginic esters in all the aforementioned sectors, especially in the medical fields, especially for the manufacture of sanitary and surgical articles.
The invention provided by the heretofore-mentioned divisional application includes also the use of total, water-insoluble alginic esters in general, that is, the new ~I

~ 338235 ones and those already described in literature, for the new applications described here, for example their use as vehicles for pharmacologically-active substances, both in the form of total, water-insoluble alginic esters with therapeutically-active alcohols, and as total, water-insoluble alginic esters of inert alcohols to mix with therapeutically-active bases as well as the pharmaceutical medicaments or preparations resulting from this use of total, water-insoluble alginic esters.
lOThe present invention further includes all the industrial articles mentioned above.
The main aspect of the present invention is therefore represented by sanitary or surgical articles provided from at least one total, water-insoluble ester of alginic acid - 15with an alcohol of the aliphatic, araliphatic, cycloaliphatic or heterocyclic series.
An aspect of the present invention is represented by the use of the new total, water-insoluble alginic esters, in substitution of the metal alginates or of the alginates of aliphatic bivalent alcohols, in their applications in the sanitary-surgical fields, and by the respective products.
An aspect of the invention provided by the heretofore-mentioned divisional application is represented by a new process for the preparation of total, water-insoluble alginic esters characterised by the treatment of a quaternary ammonium salt of alginic acid with an etherifying agent in an aprotic solvent.

G

An aspect of the invention provided by the heretofore-mentioned divisional application is represented by the use of total, water-insoluble alginic esters as vehicles for pharmaceutically-active substances and by pharmaceutical preparations or medicaments containing: 1) a pharma-cologically-active substance or an association of pharmacologically-active substances; and 2) a carrying vehicle containing a total, water-insoluble ester of alginic acid or pharmacologically-active preparation or medicaments containing a total, water-insoluble ester of alginic acid in which at least one ester group derives from an alcohol as described above.
Alcohols of the aliphatic series for use as esteri-fying components of the carboxy groups of alginic acid as taught herein are, for example, those with a maximum of 34 carbon atoms, which may be saturated or unsaturated and which may possibly also be substituted by other free or functionally modified groups, e.g. amino, hydroxy, aldehydo, keto, mercapto, carboxy groups or by groups deriving from the same, e.g. hydrocarbyl or dihydro-carbylamino [hereafter the term "hydrocarbyl" should be - taken to mean not only monovalent radicals of hydrocarbons e.g., the CnH2n+l type, but also bivalent or trivalent radicals, e.g. "alkylenes" - CnH2n - or "alkylidenes" =
CnH2n], ether or ester groups, acetal or ketal groups, thio-ether or ester thioester groups and esterified carboxy groups or carbamidic or carbamidic groups substituted by one or two hydroxy groups, by nitrile groups or by halo-gens.
In the above groups containing hydrocarbyl radicals, these are preferably lower aliphatic radicals, e.g. alkyls, with a maximum of 6 carbon atoms. These alcohols may also be interrupted in the carbon atom chain by heteroatoms, e.g. oxygen, nitrogen and sulfur. Preference is given to alcohols substituted with one or two of such functional groups.
Alcohols of the above group to be used preferentially as taught herein are those with a maximum of 12 and especially with a maximum of 6 carbon atoms and in which the hydrocarbyl radicals in the above mentioned amino, ether, ester, thioether, thioester, acetal, ketal groups representing alkyl groups with a maximum of 4 carbon atoms, and also in the esterified carboxy or substituted carba-midic groups the hydrocarbyl groups are alkyls with the same number of carbon atoms, and in which the amino or carbamidic groups may be alkyleneamino or alkylenecar-bamidic groups with a maximum of 8 carbon atoms. Of thesealcohols, those to be mentioned first and foremost are the saturated and unsubstituted ones, e.g., methyl, ethyl, propyl, isopropyl alcohols, n-butyl alcohol, isobutyl, tert-butyl alcohols, amyl, pentyl, hexyl, octyl, nonyl, and dodecyl alcohols and above all those with a linear chain, e.g., n-octyl or n-dodecyl alcohols. Of the substituted alcohols of this group, the bivalent alcohols should be listed, e.g., ethylene glycol, propylene glycol or butylene _ 23 133823~
glycol, the trivalent alcohols, e.g., glycerin, aldehydo alcohols, e.g., tartronic alcohol, carboxy alcohols, e.g., lactic acids, for example a -oxypropionic acid, glycolic acid, malic acid, tartaric acids, and citric acid, amino alcohols, e.g., aminoethanol, aminopropanol, n-aminobutanol and their dimethyl and diethyl derivatives in the aminic function, choline, pyrrolidinylethanol, piperidinylethanol, piperazinylethanol and the corresponding derivatives of n-propyl or n-butyl alcohols, monothioethylene glycol or its alkyl derivatives, for example, the ethyl derivative in the mercapto function.
of the higher saturated aliphatic alcohols, those worthy of special mention are, for example, cetyl alcohol and myricyl alcohol, but especially important as taught herein are the higher unsaturated alcohols with one or two double bonds, e.g., especially those contained in many essential oils and having an affinity with terpenes, e.g., citronellol geraniol, nerol, nerolidol, linalool, farnesol phytol.
Of the lower unsaturated alcohols, consideration should be given to propargyl alcohol.
Of the araliphatic alcohols, those to the mentioned above all are those with only one benzene residue and in which the aliphatic chain has a maximum of 4 carbon atoms, in which also the benzene residue may be substituted by between 1 and 3 methyl or hydroxy groups, or by halogen atoms, especially chlorine, bromine or iodine, and in which the aliphatic chain may be substituted by one or more _ 24 l 3 3 8 2 3 5 functional groups selected from the group consisting of free amino groups or mono-or dimethyl groups or by pyrroli-dine or piperidine groups. Of these alcohols, benzyl alcohol and phenethyl alcohol are especially preferred.
The alcohols of the cycloaliphatic or aliphatic cycloaliphatic series may derive from mono or polycyclic hydrocarbons and may have a maximum of 34 carbon atoms. Of the alcohols derived from cyclic monoanular hydrocarbons, special mention should be given to those with a maximum of 12 carbon atoms, with rings preferably containing between 5 and 7 carbon atoms, possibly substituted, for example, by between one and three lower alkyl groups, e.g. methyl, ethyl, propyl or isopropyl groups. Specific alcohols of this group are cyclohexanol, cyclohexanediol, 1,2,3-cyclo-hexanetriol and 1,3,5-cyclohexanetriol (phloroglucitol), inositol, the alcohols deriving from p-menthane, e.g., carvomenthol, menthol, ~ and ~ - terpineol, 1-terpineol, 4-terpineol and piperitol, or a mixture of these alcohols known as "terpineol", and 1,4- and 1,8-terpin. Alcohols deriving from hydrocarbons with condensed rings are, for example, those of the thujane, pinane, camphane groups, particularly thujanol, sabinol, pinol hydrate, D- and L-borneol and D- and L-isoberneol.
Polycyclic aliphatic cycloaliphatic alcohols for use in obtaining the total, water-insoluble esters of the present invention are sterols, cholic acids and steroids, e.g. sexual hormones and the synthetic analogues, in particular corticosteroids and their derivatives. Thus for G

_ 25 example it is possible to use: cholesterol, dihydro-cholesterol, epidihydrocholesterol, coprostanol, epicoprostanol, sitosterol, stigmasterol, ergosterol, cholic acid, deoxycholic acid, lithocholic acid, estriol, estradiol, equilenin, equilin and their alkyl derivatives, as well as their ethynyl propynyl derivatives in position 17, for example 17-~-ethynyl-estradiol or 7-~-methyl-17a-ethynyl-estradiol, pregnenolone, pregnanediol, testosterone and its derivatives, e.g., 17-~-methyl-1,2-dehydrotestosterone, the alkyl derivatives in position 17of testosterone and of 1,2-dehydro-testosterone, e.g., 17~-ethynyltestosterone, 17~-propynyltestosterone, norgestrel, hydroxyprogesterone, corticosterone, deoxycorticosterone, 19-nortestosterone, 19-nor-17~-methyltestosterone and 19-nor-17~ ethynyltestosterone, cortisone, hydrocortisone, prednisone, prednisolone, fludrocortisone, dexametasone, betamethasone, paramethasone, flumethasone, fluocinolone, fluprednylidene, clobetasol, beclomethasone, aldosterone, deoxycorticosterone, alphaxolone, alphadolone, bolasterone and anti-hormones, e.g., cyproterone.
Useful as esterifying components for the total, water-insoluble esters of alginic acid as taught in the above-referred-to divisional application herein are genins (aglycons) of cardioactive glycosides, e.g., digitoxigenin, gitoxigenin, digoxigenin, strophantidin, tigogenin and saponins.
Other alcohols to be used as taught in the above-referred-to divisional application are the vitamin ones, G

e.g. axerophthol, vitamins D2 and D3, aneurine, lacto-flavine, ascorbic acid, riboflavine, thiamine, pantothenic acid.
Of the heterocyclic alcohols, the following are preferred: furfuryl alcohol, alkaloids and derivatives, e.g., atropine, scopolamine, cinchonine, cinchonidine, quinine, morphine, codeine, nalorphine, N-butylscopol-ammonium bromide, ajmaline; phenylethylamines, e.g., ephedrine, isoproterenol, epinephrine; phenothiazine drugs, e.g., perphenazine, pipothiazine, carphenazine, homo-fenazine, acetophenazine, fluphenazine, N-hydroxyethyl-promethazine chloride; thioxanthene, drugs, e.g., flupen-thixol, clopenthixol; anticonvulsants, e.g., meprophendiol, antipsychotic drugs, e.g., opipramol; antiemetics, e.g., oxypendyl; analgesics, e.g., carbetidine, phenoperidine and methadol; hypnotics, e.g., etodroxizine; anorexics, e.g., benzhydrol and diphemethoxidine; muscle relaxants, e.g., cinnamedrine, diphylline, mephenesin, methocarbamol, chlorphenesin, 2,2-diethyl-1,3-propanediol, quaifenesin, idrocilamide; coronary vasodilators, e.g., dipyridamole and oxyfedrine; adrenergic blockers, e.g., propanolol, timolol, pindolol, bupranolol, atenolol, metoprolol, practolol;
antineoplastics, e.g., 6-axauridine, cytarabine, floxuridine; antibiotics, e.g., chloramphenicol, thiamphenicol, erythromycin, oleandomycin, lincomycin;
antivirals, e.g., idoxuridine; peripheral vasodilators, e.g., isonicotinyl alcohol; carbonic anhydrase inhibitors, e.g., sulocarbilate; anti-asthmatics and anti-inflammatories, e.g., tiaramide; sulfamidics, e.g., 2-p-sulfanylanilinoethanol.
The total, water-insoluble esters of alginic acid as taught herein have the following general formula:

XoRl O ~-o ~ O
- I H ~Y H H Y

wherein Rl and R2 are each independently hydrogen or an alcoholic moiety selected from the group consisting of aliphatic, araliphatic, cycloaliphatic and heterocyclic radicals with the proviso that the total, water-insoluble ester is not an ester of methyl alcohol.
As discussed above, in some cases, total, water-insoluble alginic acid esters in which the ester groups derive from one or more hydroxy substances with therapeutic action, may be of special interest, and naturally include all possible variations of the same. Especially interesting are those substances in which two different types of ester groups deriving from drugs of a hydroxy character are present. In particular, it is possible to have total, water-insoluble alginic esters deriving, on the one hand from an anti-inflammatory steroid, e.g. one of those mentioned above, and on the other hand from a vitamin, from an alkaloid or from antibiotic, e.g. one of those listed here.

G

The degree of esterification of alginic acid with the above-mentioned alcohols depends first and foremost on the special properties desired from the various fields of application. For example, a greater or lesser degree of lipophilia or hydrophilia with regard to such tissues, for example, the skin. Usually, a high degree of esterifica-tion to the point of total esterification of alginic acid increases its lipophilic character and therefore decreases its solubility in water, and this provides total, water-insoluble esters useful in the present invention. For ause in therapy according to the present invention of the new total, water-insoluble esters of the invention provided by the heretofore-mentioned divisional application, for example, it is of the utmost importance to regulate the degree of esterification in order to ensure good and increased lipophilia compared to metal alginates.
Naturally, it is necessary to consider also the influence of the molecular size of the same esterifying component, which usually has an inversely proportional influence on hydrosolubility.
As has been disclosed previously, esterification of the carboxy groups of alginic acid may play several roles to be exploited in various fields, for example in medicine, using the total, water-insoluble esters as therapeutic agents or in surgery using them as plastic articles. For use in therapy, esterification of an alcohol can in itself be considered therapeutically-active, e.g., anti-C~

29inflammatory corticosteroids, for example, with alginic acid as a means of improving therapeutic efficacy.
With regard to similar therapeutically-active alcohols, alginic acid therefore acts as a particularly-efficient vehicle which is compatible with the biologicalenvironment. Many of these pharmacologically-active alcohols appear in the above list of alcohols for use in esterification as taught herein and the possible appli-cations of the corresponding total, water-insoluble esters therefore are evident, since their indications are the same as those for the free alcohols. Again, as has already been said, in partial esters with therapeutically-active alcohols, it is possible to esterify part or all of the remaining carboxy groups of the alginic component with pharmacologically-inert alcohols, for example saturated lower aliphatic alcohols, for example, ethyl or isopropyl alcohols to provide total, water-insoluble esters.
One particularly interesting aspect of the invention provided by the heretofore-mentioned divisional application is the possibility of preparing more stable drugs than the available up to now. It is possible for example to obtain drugs with a "retard" action with total, water-insoluble alginic esters with therapeutically active alcohols.
For cosmetic purposes, it is preferable to use total, water-insoluble esters of alginic acid with pharmacologi-cally-inert alcohols, for example, saturated or unsaturated aliphatic alcohols, for example, unsubstituted alcohols of this type with straight or ramified chains, for example G

between 1 and 8 carbon atoms, e.g. those specifically mentioned. Of particular interest also are unsaturated alcohols, for example with one or more double bonds, e.g., vinyl or allyl alcohols, and the condensed derivatives, e.g., especially polyvinyl alcohol or polyvalent alcohols, e.g., glycerin. In this case, also, mixed total, water-insoluble esters may be used according to the particular use for which they are intended.
Cycloaliphatic alcohols are also useful, for example, those derived from cyclopentane or cyclohexane and from their derivatives which are substituted by lower alkyl groups, for example, alkyls with between 1 and 4 carbon atoms, especially from methyl groups. Particularly interesting are total, water-insoluble esters with cycloaliphatic and aliphatic-cycloaliphatic alcohols derived from terpenes, those mentioned above, and from therapeutically-active alcohols, which can otherwise be used in cosmetics.
The alcohols to be used preferably for the manufacture of sanitary and surgical articles according to the present invention are essentially the same as those mentioned above for cosmetic use. For the manufacture of sanitary-surgical articles, total water-insoluble esters are used.
While not an aspect of the present invention, the present disclosure teaches salts with organic bases, especially azotized bases and, therefore, aliphatic, araliphatic, cycloaliphatic or heterocyclic amines. These ammonium salts may derive rom therapeutically-acceptable _ 31 amines or nontoxic but therapeutically-inactive amines, or from amines with a therapeutic action. The first type are aliphatic amines, for example mono-, di- and tri-alkyl-amines with alkyl groups with a maximum of 8 carbon atoms or arylalkylamines with the same number of carbon atoms in the aliphatic part and where aryl means a benzene group possibly substituted by between 1 and 3 methyl groups or halogen atoms or hydroxy groups. The biologically-inactive bases for the formation of the salts may also be cyclic, e.g., monocyclic alkyleneamines with rings of between 4 and 6 carbon atoms, possibly interrupted in their ring by heteroatoms selected from the group consisting of nitrogen, oxygen and sulfur, e.g., piperazine or morpholine, or may be substituted, for example by amino or hydroxy functions e.g. aminoethanol, ethylenediamol, ethylenediamine, ephedrine or choline.
The biologically-active amines to be used for salifi-cation and whose therapeutic action may be put to use are all known azotized and basic drugs, e.g., those in the following groups: alkaloids, peptides, phenothiazine, benzodiazepine, thioxanthenes, hormones, vitamins, anticonvulsants, antipsychotics, antiemetics, anesthetics, hypnotics, anorexics, tranquilizers, muscle relaxants, coronary vasodilators, antineoplastics, antibiotics, antibacterials, antivirals, antimalarials, carbonic anhydrase inhibitators, nonsteroid anti-inflammatories, vasoconstrictors, cholinergic agonists, cholinergic G--32 l 338235 antagonists, adrenergic agonists, adrenergic antagonists, narcotic antagonists.
Examples of specific useful drugs are all those drugs mentioned above having azotized basic groups regarding the total, water-insoluble alginic esters with therapeutically-active alcohols or those mentioned hereafter for example the various antibiotics.
The vehicling action of total, water-insoluble alginic esters opens up possibilities for new medicaments wherein the components are: 1) a pharmacologically-action substance or an association or mixture of two or more such substances; and 2) a total, water-insoluble alginic ester as described above.
As provided in the above-mentioned divisional application the total, water-insoluble alginic esters for use in these medicaments are, above all, those in which the esterifying alcohol is itself not pharmacologically-active, for example, a simple aliphatic alcohol, as described above. Included, however, are medicaments of this type in which the total, water-insoluble ester is also pharmaceuti-cally-active, for example in the case of one of the total, water-insoluble esters described above deriving from pharmacologically-active alcohols.
As provided in the above-mentioned divisional appli-cation the use of total, water-insoluble alginic esters as a vehicle is particularly useful in ophthalmology, where it is possible to observe a particular compatibility of the new products with the corneal epithelium, thereby showing `- 1 338235 excellent tolerability, with no sensitization effect.
Furthermore, when the medicaments are administered in the form of concentrated solution with elastic-viscous characteristics or in solid form, it is possible to obtain transparent, homogenous and stable films on the corneal epithelium with excellent adhesive qualities, guaranteeing prolonged bioavailability of the drug and therefore representing first class products with a retard effect.
These ophthalmic medicaments are especially valuable in the veterinary field, considering that there are no veterinary preparations for ophthalmic use containing chemical agents.
Usually, preparations intended for human use are utilized, and sometimes these do not guarantee a specific range of action or they do not allow for the particular conditions in which treatment must take place. This is the case, for example, of infective keratoconjunctivitis, pink eye or IBK, an infection which usually afflicts cattle, sheep and goats. Presumably for these three species there exist specific etiological factors. More precisely, in cattle the main microorganism involved seems to be Moraxella bovis (even though other agents of a viral origin should not be excluded, for example the Rinotracheitis virus, Micoplasma in sheep, Rickettsia and ChlamYdia, Rickettsia in goats).
The disease occurs in an acute form and tends to spread rapidly: in the initial stages, the symptomatology is characterised by blepharospasm and excessive watering of the eye, followed by purulent exudate, conjunctivitis and keratitis, often associated with high temperature, reduced _ 34 1 338235 appetite and reduced milk production. Particularly serious are the corneal lesions which in their final stages may even result in perforation of the cornea itself. The clinical course varies from a few days to several weeks.
A wide range of treatments based on chemical agents are used, administered both topically (often associated with steroid anti-inflammatories), and systemically. Examples of these are: tetracyclines, as oxytetracycline, peni-cillins, e.g. cloxacillin and benzylpenicillin, sulfamides, polymyxin B (associated with miconazole and prednisolone), chloramphenicol and tilosina. Topical treatment of the disease, despite its apparent simplicity, is still an open problem, since for one reason or another, with the ophthal-mic preparations in use heretofore it has not been possible to obtain therapeutically-efficient concentrations of anti-biotic or sulfamidic in the lachrymal secretion. This is quite understandable in the case of solutions, if one thinks of the mainly inclined position of the head in the above-mentioned animals, but it is also true of the semisolid medicaments since the excipients commonly used in them do not have the necessary qualities of adhesion to the corneal surface, lacking generally a sufficiently high concentration of active substance and being unable to obtain perfect distribution of the same (presence of a distribution gradient). These drawbacks to conventional collyriums in use in ophthalmology have for example been described by Slatter et al. in "Austr.Vet.J.," 1982, 59 (3), pp. 69-72.

l 3 3 8 2 3 5 By using the total, water-insoluble esters described herein, and as provided in the above-referred-to divisional application, these difficulties can be overcome. The presence of the total, water-insoluble alginic ester as vehicle in ophthalmic drugs allows for the formulation of excellent preparations with no concentration gradient of the active substance and therefore with homogeneity, transparency and excellent adhesion to the corneal epithelium, with no sensitisation effects, with excellent vehicling of the active substance and possibly with a retard effect.
The above-mentioned properties of the new medicaments may of course also be used to advantage in fields other than ophthalmology: they may be applied in dermatology and in infections of the mucus, for example of the mouth. They may also be used to obtain a systemic effect thanks to transcutaneous absorption, for example in suppositories.
All these applications are possible both in human and veterinary medicine. In human medicine, the new medicament is particularly suitable for use in pediatrics. The invention provided by the heretofore-mentioned divisional application therefore also includes in particular any one of these therapeutic applications.
For the sake of brevity, in the following text reference to the active substance of component (1) as taught herein should be understood to include the associa-tion or mixture of two or more active substances.

~ 36 1338235 Component (1) as described above is a pharmaco-logically-active substance. Such substances can first of all be generically catalogued with respect to their use in the various fields of therapy, beginning with the distinc-tion between human and veterinary medicine, and then specifying the various sectors of application with respect to the organs or tissues to be treated, ophthalmology, dermatology, otolaryngology, gynecology, angiology, neurology, or any type of pathology of internal organs with can be treated by topical application, for example, rectal applications. According to one particular aspect of the invention provided by the heretofore-mentioned divisional application, the pharmacologically-active substance (1) is first and foremost a substance for ophthalmic use.
According to a further criterion, the pharmacologically-active substance (1) should be identified according to its effect and can therefore, for example, be an anesthetic, analgesic, anti-inflammatory, vasoconstrictor, antibac-terial, or antiviral drug. In the field of ophthalmology, the indications can, in particular, be for example: miotic, anti-inflammatory, wound healing and antimicrobial effects.
Component (1) may also be, according to the invention provided by the heretofore-mentioned divisional applica-tion, an association of two or more active substances, as contained in many known medicaments. For example, in ophthalmology, it is possible to associate an antibiotic with an antiphlogistic and a vasoconstrictor or several antibiotics with one or more antiphlogistics, or one or _ 37 1 338235 more antibiotics with a mydriatic or a myotic or wound healer or an anti-allergic agent, etc. For example, it is possible to use the following associations of ophthalmic drugs: kanamycin + phenylephrine + dexamethasone phos-phate, kanamycin + betamethasone phosphate + phenylephrine,or similar associations with other antibiotics used in ophthalmology, e.g. rolitetracycline, neomycin, gentamycin, tetracycline.
In dermatology it is possible to use, as active component (1), associations of various antibiotics, e.g., erythromycin, gentamycin, neomycin, gramicidin, polymyxin B, between themselves, or such antibiotics with anti-inflammatory agents, for example corticosteroids, for example hydrocortisone + neomycin, hydrocortisone +
neomycin + polymyxin B + gramicidin, dexamethasone +
neomycin, fluorometholone + neomycin, prednisolone +
neomycin, triamcinolone + neomycin + gramicidin + nystatin, or any other association used heretofore in conventional dermatological preparations. The associations of various active substances are not, of course, limited to these fields, but in all the above sectors of medicine it is possible to use associations similar to those already in use for the pharmaceutical preparations known to the art.
According to one particular aspect of the invention provided by the heretofore-mentioned divisional applica-tion, it is possible to prepare the medicaments of this type starting with the previously isolated and possibly purified salts and, in their solid anhydrous state, as an - 38 l 338235 amorphous powder, which on contact with the tissue to be treated constitute a concentrated aqueous solution of a gelatinous character with viscous consistency and elastic properties. These qualities are also maintained at stronger dilutions and it is therefore possible to use, instead of the above anhydrous salts, solutions more or less concentrated in water or saline, possibly with the addition of other excipients or additives, e.g., other mineral salts to regulate the pH and osmotic pressure. It is also possible, of course, to use salts for the prepara-tion of gels, inserts, creams or ointments, containing other excipients or ingredients used in traditional formu-lations of these pharmaceutical preparations.
According to a main aspect of the invention, provided by the heretofore-mentioned divisional application, how-ever, the medicaments containing the total, water-insoluble alginic ester are used with therapeutically-active or inactive substances as a vehicle alone (excepting possibly an aqueous solvent). Also included in the invention provided by the heretofore-mentioned divisional application are the mixtures obtainable from all types of medicaments described here and also mixtures of such medicaments, as well as possibly mixtures of the new total, water-insoluble alginic esters with free alginic acid.
Examples of pharmacologically-active substances (1) which may be used in ophthalmic medicaments according to the invention provided by the heretofore-mentioned divi-sional application are: basic and non-basic antibiotics, for example, aminoglycosides, macrolides, tetracyclines and peptides, e.g., gentamycin, neomycin, streptomycin, dihydrostreptomycin, kanamycin, amikacin, tobramycin, spectinomycin, erythromycin, oleandomycin, carbomycin, spiramycin, oxytetracycline, rolitetracycline, bacitracin, polymyxin B, gramicidin, colistin, chloramphenicol, linomycin, vancomycin, novabiocin, ristocetin, clindamycin, amphotericin B, griseofulvin, and nystatin and possibly their salts, e.g., sulfates or nitrates, or associations of these between themselves or with other active principles, e.g., those mentioned hereafter.
Other ophthalmic drugs which may be used to advantage according to the invention provided by the heretofore-mentioned divisional application are: other anti-infec-tives, e.g. diethylcarbamazine, mebendazole, sulfamidics,e.g. sulfacetamide, sulfadiazine, sulfisoxazole; antivirals and anti-tumorals, e.g.iododeoxyuridine, adenine arabino-side, trifluorothymidine, acyclovir, ethyldeoxyuridine, bromovinyldeoxyuridine, 5-iodo-5'-amino-2',5'-dideoxy-uridine; steroid anti-inflammatory agents, e.g., dexametha-sone, hydrocortisone, prednisolone, fluorometholone, medri-sone and possibly their esters, for example, phosphoric acid esters; nonsteroid anti-inflammatories, for example, indomethacin, oxyphenbutazone, flurbiprofen; wound healers, e.g., epidermal growth factor EGF; local anesthetics, e.g., benoxinate, proparacaine and possibly their salts;
cholinergic agonists, e.g., pilocarpine, methacholien, carbamylcholine, aceclidine, physostigmine, neostigmine, and demecarium and possibly their salts; cholinergic antagonist drugs, e.g., stropine and its salts; adrenergic agonist drugs, e.g., noradrenaline, adrenalin, naphazoline, methoxamine and possibly their salts; adrenergic antagonist drugs e.g. propanolol, timolol, pindolol, bupranolol, atenolol, metoprolol, oxprenolol, practolol, butoxamine, sotalol, butethrin, and labetalol and possibly their salts.
Associations or mixtures of such drugs between themselves and possibly with other principles may also be used as component (1) according to the invention provided by the heretofore-mentioned divisional application if instead of only one active substance (1), associations of active substances are used, e.g., the reported above, the salts of the basic active substances and the partial ester of alginic acid may be mixed salts of one or more of such basic substances or possibly mixed salts of this type with a certain number of further acid groups of the polysac-charide salified with the above mentioned metals or bases.
For example, it is possible to prepare salts of total, water-insoluble esters of alginic acid with a pharma-cologically-inactive alcohol, for example a lower alkanol, and with a certain percentage of the acid groups salified with the antibiotic kanamycin, another percentage salified with the vasoconstrictor phenylephrine, and a remaining percentage of the free acid groups being possibly salified, for example, with sodium or one of the other above mentioned metals. It is possible to mix this type of mixed salt too, with free alginic acid or its fractions or their metal salts, as indicated above for the medicaments constituted by salts of only one active substance with the above-described polysaccharide total, water-insoluble esters.
Examples of active substances which may be used in this aspect of the invention provided by the heretofore-mentioned divisional application on their own or in association between themselves or with other active principles in dermatology are: therapeutic agents, e.g., anti-infective, antibiotic, antimicrobial, anti-inflammatory, cytostatic, cytotoxic antiviral, anesthetic agents, and prophylactic agents, e.g. sun shields, deodorants, antiseptics and disinfectants. of the anti-biotics, may be mentioned erythromycin, bacitracin, géntamycin, neomycin, aureomycin, gramicidin and associa-tions of the same, antibacterials and disinfectants, nitrofurazone, mafenide, chlorhexidine, and 8-hydroxy-quinoline derivatives and possibly their salts; anti-inflammatories, above all corticosteroids, e.g., prednisolone, dexamethasone, flumethasone, clobetasol, acetonide of triamcinolone, betamethasone or their esters, e.g. valerianates, benzoates, and diproprionates; of the cytotoxics, fluorouracil, methotrexate, and podophyllin; or of the anesthetics, dibucaine, lidocaine,or benzocaine.
This list is of course only for exemplary purposes and any other agents described in literature may be used.
From the examples discussed for ophthalmology and dermatology, it is possible to determine by analogy which ~ 42 1 338235 medicaments according to the invention provided by the heretofore-mentioned divisional application may be used in the other fields of medicine mentioned above, e.g., otolaryngology or odontology or in internal medicine. For example, in endocrinology, it is possible to use prepara-tions absorbed intradermally or through the mucus, for example, by rectal or nasal absorption, e.g., nasal sprays or preparations for inhalation into the oral cavity or pharynx. These preparations may therefore be, for example, anti-inflammatories, or vasoconstrictors or vasopressors, e.g., those already mentioned for ophthalmology, vitamins, antibiotics, e.g. those mentioned above, hormones, chemo-therapeutics, antibacterials, etc., again as mentioned above for use in dermatology.
According to the chemically new and original procedure described herein and claimed in the invention provided by the heretofore-mentioned divisional application, the total, water-insoluble alginic acid esters may be prepared to advantage starting with quaternary ammonium salts of alginic acid with an etherifying agent in a preferably aprotic organic solvent, e.g. dialkylsulfoxides, dialkyl-carboxamides, e.g. in particular lower alkyl dialkyl-sulfoxides, above all dimethylsulfoxide, and lower alkyl dialkylamides of lower aliphatic acids, e.g. dimethyl or diethyl formamide or dimethyl or diethylacetamide. It is possible, however, to use other solvents which are not always aprotic, e.g., alcohols, ethers, ketones, esters, especially aliphatic or heterocyclic alcohols and ketones with a low boiling point, e.g. hexafluoroisopropanol and trifluoroethanol. The reaction is brought about preferably at a temperature of between 0 and 100C, and especially between 25 and 75, for example at 30.
Esterification is preferably carried out by gradually adding the esterifying agent to the above-mentioned ammonium salt dissolved in one of the solvents mentioned, for example, in dimethylsulfoxide. As alkylating agents, those mentioned above can be used, especially hydrocarbyl halides, for example, alkyl halides.
The preferred esterification process, therefore, comprises reacting, in an organic solvent, a quaternary ammonium salt of alginic acid with a stoichiometric quantity of a compound of the formula:
A-X, wherein A is selected from the group consisting of an aliphatic, araliphatic, cycloaliphatic, aliphatic-cyclo-aliphatic and heterocyclic radicals and X is a halogen atom, and wherein the stoichiometric quantity of A-X is determined by the degree of esterification desired.
As starting quaternary ammonium salts, it is preferable to use lower ammonium tetraalkylates, the alkyl groups having preferably between 1 and 6 carbon atoms.
Mostly, the alginate of tetrabutylammonium is used. These quaternary ammonium salts can be prepared by reacting a metal salt of alginic acid, preferably one of those mentioned above, especially a sodium or potassium salt, in aqueous solution with a sulfonic resin salified with the _ 44 1 338235 quaternary ammonium base. The tetraalkyl- ammonium alginates deriving from lower alkyls, especially alkyls with between 1 and 6 carbon atoms, are new and form another aspect of the invention provided by the heretofore-mentioned divisional application. Unexpectedly, thesesalts proved to be soluble in the above aprotic solvents, and esterification of alginic acid according to the new procedure is therefore made particularly easy and gives abundant yields. Only by using this procedure, therefore, is it possible exactly to dose the number of carboxy groups of alginic acid to be esterified.
One variation of the previously specified procedure consists in reacting a potassium or sodium salt of alginic acid, suspended in a suitable solution, e.g., dimethylsul-foxide, with a suitable alkylating agent in the presence ofa catalyzing quantity of a quaternary ammonium salt, e.g., tetrabutylammonium iodide. The new procedure makes it possible to obtain, as already stated, the total, water-insoluble esters of alginic acid and also substituted alcohols, e.g., glycols, which were previously unobtainable.
To prepare new total, water-insoluble esters according to the invention provided by the heretofore-mentioned divisional application, it is possible to use alginic acids of any origin, for example, the acids extracted from the above-mentioned natural starting materials. The preparation of these acids is described in literature: it is preferable to use purified alginic acids.

G

_ 45 The present disclosure also teaches modifications of the preparation procedures of the new total, water-insoluble esters in which a procedure is interrupted at any stage or which start with an intermediate compound followed by the remaining stages, or in which the starting products are formed in situ.
The following Examples do not in any way limit the scope of the present disclosure.
Example 1 - Preparation of the tetrabutYlammonium salt of alginic acid.
lOm.Eq. of sodium salt of alginic acid, corresponding to 2g. of dry compound, are solubilized in 300 ml of distilled water. The solution is then passed through a thermostatic column at 4C containing 15 ml of sulfonic resin (e.g. that known by the Trade-mark DOWEX~ 50x8) in the form of tetrabutylammonium. The sodium-free eluate is frozen and freeze-dried.
Yield 3.3 g.
ExamPle 2 - PreParation of the (partial) ethYl ester of alqinic acid - 10% of the carboxy qrouPs esterified - 90%
of the carboxY groups salified.
10 g (23.9 m.Eg.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from Laminaria hyperborea) are solubilized in 400 ml of DMSO at 25C. 0.377 g (2.39 m.Eg.) of ethyl iodide are added.

1 33823~

The solution is well agitated for 12 hours at 30C.
a) To completely convert the carboxy salts of tetrabutylammonium residues to sodium salt form, to the resulting solution is added 2.5 g of NaCl dissolved in 50 ml of distilled H2O, cooling it from the outside in a bath of H2O~ice.
The solution is slowly poured by regular drops and under agitation in 2000 ml of ethyl acetate.
The precipitate is separated by filtration, washed three times with 100 ml of acetone/H2O
5:1 and 3 times with 100 ml of pure acetone, then vacuum dried.
Yield: 6 g.
b) To convert the carboxy salts of tetrabutyl-ammonium residues to calcium salt form, the procedure is as above, substituting calcium chloride for the sodium chloride.
Yield: 6.1 g.
Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

ExamPle 3 - Preparation of the (partial) ethyl ester of alqinic acid - 30% of the carboxy groups esterified -70% of the carboxY grouPs salified.
10 g (23.9 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from AscoPhyllum nodosum) are solubilized in 400 ml of DMSO

_ 47 _ 1 3 3 8 2 3 5 at 25C. 1.31 g (7.18 m.Eq.) of ethyl iodide are added.
The solution is well agitated for 12 hours at 30C.
a) For complete conversion of the carboxy salts of tetrabutylammonium residues to sodium salt, to the resulting solution is added 2.5 g of NaCl dissolved in 50 ml of distilled H2O, cooled from the outside with a bath of H2O/ice.
The solution is slowly poured by regular drops and under agitation in 2000 ml of ethyl acetate.
The precipitate is separated by filtration, washed three times with 100 ml of acetone/H2O
S:l and 3 times with 100 ml of pure acetone, then vacuum dried.
Yield: 5 g.
b) To convert the carboxy salt of tetrabutylammonium residues to calcium salts, the procedure is as above, substituting calcium chloride for the sodium chloride.
Yield: 5.1 g.
Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

Example 4 - PreParation of the (partial) ethyl ester of alginic acid - 50% of the carboxy qroups esterified -50% of the carboxy qroups salified.
10 g (23.9 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from J . I ~ - ' ;" . . :' ' -MacrocYstis pyrifera) are solubilized in 400 ml of DMSO
at 25C. 1.88 g (11.9 m.Eq.) of ethyl iodide are added.
The solution is well agitated for 12 hours at 30C.
a) For complete conversion of the carboxy salts of tetrabutylammonium residues to sodium salt, to the resulting solution is added 2.5 g of NaCl dissolved in 50 ml of distilled H2O, cooled from the outside with a bath of H2O/ice.
The solution is slowly poured by regular drops and under agitation in 2000 ml of ethyl acetate.
The precipitate is separated by filtration, washed three times with 100 ml of acetone/H2O
5:1 and 3 times with 100 ml of pure acetone, then vacuum dried.
Yield: 4.5 g.
b) To convert the carboxy salt of tetrabutylammo-nium residues to calcium salts, the procedure is as above, substituting calcium chloride for the sodium chloride.
Yield: 4.6 g.
Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

Example 5 - Preparation of the (partial) ethYl ester of alqinic acid - 70% of the carboxy qroups esterified -30% of the carboxY qroups salified.
10 g (23.9 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from -1 33823~

Laminaria hyPerborea) are solubilized in 400 ml of DMSO
at 25C. 2.64 g (16.7 m.Eq.) of ethyl iodide are added.
The solution is well agitated for 12 hours at 30C.
a) For complete conversion of the carboxy salts of tetrabutylammonium residues to sodium salt, to the resulting solution is added 2.5 g of NaCl dissolved in 50 ml of distilled H2O, cooled from the outside with a bath of H2O/ice.
The solution is slowly poured by regular drops and under agitation in 2000 ml of ethyl acetate.
The precipitate is separated by filtration, washed three times with 100 ml of acetone/H2O
5:1 and 3 times with 100 ml of pure acetone, then vacuum dried.
Yield: 4 g.
b) To convert the carboxy salt of tetrabutylammo-nium residues to calcium salts, the procedure is as above, substituting calcium chloride for the sodium chloride.
Yield: 4.2 g.
Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

Example 6 - PreParation of the (partial) ethyl ester of alqinic acid - 90% of the carboxY grouPs esterified -10% of the carboxy qrouPs salified.
10 g (23.9 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from -.

Macrocystis pYrifera) are solubilized in 400 ml of DMSO
at 25C. 3.39 g (21,5 m.Eq.) of ethyl iodide are added.
The solution is well agitated for 12 hours at 30C.
a) For complete conversion of the carboxy salts of tetrabutylammonium residues to sodium salt, to the resulting solution is added 2,5 g of NaCl dissolved in 50 ml of distilled H2O, cooled from the outside with a bath of H2O/ice.
The solution is slowly poured by regular drops and under agitation in 2000 ml of ethyl acetate.
The precipitate is separated by filtration, washed 3 times with 100 ml of acetone/H2O 5:1 and 3 times with 100 ml of pure acetone, then vacuum dried.
Yield: 5.5 g.
b) To convert the carboxy salt of tetrabutylammo-nium residues to calcium salts, the procedure is - as above, substituting calcium chloride for the sodium chloride.
Yield: 5.6 g.
Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

Example 7 - Preparation of the (partial) isoproPYl ester of alqinic acid - 90% of the carboxY qroups esterified -10% of the carboxy grouPs salified.
10 g (23.9 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from 1 33823~

AscoPhyllum nodosum) are solubilized in 400 ml of DMSO
at 25C. 3.73 g (21.5 m.Eq.) of isopropyl iodide are added.
The solution is well agitated for 12 hours at 30C.
a) For complete conversion of the carboxy salts of tetrabutylammonium residues to sodium salt, to the resulting solution is added 2.5 g of NaCl dissolved in 50 ml of distilled H2O, cooled from the outside with a bath of H2O/ice.
The solution is slowly poured by regular drops and under agitation in 2000 ml of ethyl acetate.
The precipitate is separated by filtration, washed 3 times with 100 ml of acetone/H2O 5:1 and 3 times with 100 ml of pure acetone, then vacuum dried.
Yield: 4.2 g.
b) To convert the carboxy salt of tetrabutylammo-nium residues in calcium salts, the procedure is as above, substituting the sodium chloride for calcium chloride.
Yield: 4 g.
Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

ExamPle 8 - PreParation of the (partial) isopropYl ester of alqinic acid - 70~ of the carboxy grouPs esterified -30% of the carboxy qroups salified.
10 g (23.9 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from Laminaria hYperborea) are solubilized in 400 ml of DMSO
at 25C. 2.9 g (16.7 m.Eq.) of isopropyl iodide are added.
The solution is well agitated for 12 hours at 30C.
a) For complete conversion of the carboxy salts of tetrabutylammonium residues to sodium salt, to the resulting solution is added 2.5 g of NaCl dissolved in 50 ml of distilled H2O, cooled from the outside with a bath of H2O/ice.
The solution is slowly poured by regular drops and under agitation into 2000 ml of ethyl acetate. The precipitate is separated by filtra-tion, washed 3 times with 100 ml of acetone/
H2O 5:1 and 3 times with lob ml of pure acetone, then vacuum dried.
Yield: 4 g.
b) To convert the carboxy salts of tetrabutylammo-nium residues in calcium salts, the procedure is as above, substituting the sodium chloride for calcium chloride.
Yield: 3.8 g.
Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

Example 9 - PreParation of the (partial) isopropyl ester of alginic acid - 50% of the carboxY qroups esterified -50% of the carboxy qroups salified.
10 g (23.9 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from _ 53 _ 1 ~ 3 8 2 3 5 Macrocystis pYrifera) are solubilized in 400 ml of DMSO
at 25C. 2.07 g (11.9 m.Eq.) of isopropyl iodide are added.
The solution is well agitated for 12 hours at 30C.
a) For complete conversion of the carboxy salts of tetrabutylammonium residues to sodium salt, to the resulting solution is added 2.5 g of NaCl dissolved in 50 ml of distilled H2O, cooled from the outside with a bath of H2O/ice.
The solution is slowly poured by regular drops and under agitation into 2000 ml of ethyl acetate. The precipitate is separated by filtration, washed 3 times with 100 ml of acetone/H2O 5:1 and 3 times with 100 ml of pure acetone, then vacuum dried.
Yield: 4.2 g.
b) To convert the carboxy salt of tetrabutylammo-nium residues in calcium salts, the procedure is as above, substituting the sodium chloride for calcium chloride.
Yield: 4.2 g.
Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

Example 10 - PreParation of the (partial) isopropyl ester of alginic acid - 30% of the carboxY qrou~s esterified - 70% of the carboxy groups salified.
10 g (23.9 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from - - . ~ . .

-AscophYllum nodosum) are solubilized in 400 ml of DMSO
at 25C. 1.24 g (7.18 m.Eq.) of isopropyl iodide are added.
The solution is well agitated for 12 hours at 30C.
a) For complete conversion of the carboxy salts of tetrabutylammonium residues to sodium salt, to the resulting solution is added 2.5 g of NaCl dissolved in 50 ml of distilled H2O, cooled from the outside with a bath of H2O/ice.
The solution is slowly poured by regular drops and under agitation into 2000 ml of ethyl acetate. The precipitate is separated by filtration, washed 3 times with 100 ml of acetone/H2O 5:1 and 3 times with 100 ml of pure acetone, then vacuum dried.
Yield: 5.5 g.
b) To convert the carboxy salt of tetrabutylammo-nium residues in calcium salts, the procedure is as above, substituting the sodium chloride for calcium chloride.
Yield: 5.4 g.
Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

Example 11 - Preparation of the (partial) isoproPYl ester of alqinic acid - 10% of the carboxy groups esterified - 90% of the carboxY qrouPs salified.
10 g (23.9 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from -_ 55 _ 1 33823~

Laminaria hYperborea) are solubilized in 400 ml of DMSO
at 25C. 0.42 g (2.3 m.Eq.) of isopropyl iodide are added.
The solution is well agitated for 12 hours at 30C.
a) For complete conversion of the carboxy salts of tetrabutylammonium residues to sodium salt, to the resulting solution is added 2.5 g of NaCl dissolved in 50 ml of distilled H2O, cooled from the outside with a bath of H2O/ice.
The solution is slowly poured by regular drops and under agitation in 2000 ml of ethyl acetate.
The precipitate is separated by filtration, washed 3 times with 100 ml of acetone/H2O 5:1 and 3 times with 100 ml of pure acetone, then vacuum dried.
Yield: 5.8 g.
b) To convert the carboxy salt of tetrabutylammo-nium residues in calcium salts, the procedure is as above, substituting the sodium chloride for calcium chloride.
Yield: 5.8 g.
Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

Example 12 - Preparation of the (partial) terbutyl ester of alqinic acid - 90% of the carboxy groups esterified -10% of the carboxY qroups salified.
10 g (23.9 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from - 56 - 1 3 3 8 2 3 ~

AscoPhyllum nodosum) are solubilized in 400 ml of DMSO
at 25C. 4.1 g (21.5 m.Eq.) of terbutyl iodide are added.
The solution is well agitated for 12 hours at 30C.
a) For complete conversion of the carboxy salts of tetrabutylammonium residues to sodium salt, to the resulting solution is added 2.5 g of NaCl dissolved in 50 ml of distilled H2O, cooled from the outside with a bath of H2O/ice.
The solution is slowly poured by regular drops and under agitation into 2000 ml of ethyl acetate. The precipitate is separated by filtration, washed 3 times with 100 ml of acetone/H2O 5:1 and 3 times with 100 ml of pure acetone, then vacuum dried.
Yield: 4 g.
b) To convert the carboxy salt of tetrabutylammo-nium residues in calcium salts, the procedure is as above, substituting the sodium chloride for calcium chloride.
Yield: 4.1 g.
Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

Example 13 - Preparation of the (Partial) terbutyl ester of alqinic acid - 70% of the carboxy qroups esterified -30% of the carboxY qrouPs salified.
10 g (23.9 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from - 57 _ 1 3 3 8 2 3 ~

Laminaria hYperborea) are solubilized in 400 ml of DMSO
at 25C. 3.14 g (16.7 m.Eq.) of terbutyl iodide are added.
The solution is well agitated for 12 hours at 30C.
a) For complete conversion of the carboxy salts of tetrabutylammonium residues to sodium salt, to the resulting solution is added 2,5 g of NaCl dissolved in 50 ml of distilled H2O, cooled from the outside with a bath of H2O/ice.
The solution is slowly poured by regular drops and under agitation in 2000 ml of ethyl acetate.
The precipitate is separated by filtration, washed 3 times with 100 ml of acetone/H2O 5:1 and 3 times with 100 ml of pure acetone, then vacuum dried.
Yield: 5 g.
b) To convert the carboxy salt of tetrabutylammo-nium residues in calcium salts, the procedure is as above, substituting the sodium chloride for calcium chloride.
Yield: 5 g.
Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

Example 14 - Preparation of the (partial) terbutyl ester of alginic acid - 50% of the carboxY grouPs esterified -50% of the carboxY qroups salified.
10 g (23.9 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from --Macrocystis pyrifera) are solubilized in 400 ml of DMSO
at 25C. 2.25 g (11.9 m.Eq.) of terbutyl iodide are added.
The solution is well agitated for 12 hours at 30C.
a) For complete conversion of the carboxy salts of tetrabutylammonium residues to sodium salt, to the resulting solution is added 2.5 g of NaCl dissolved in 50 ml of distilled H2O, cooled from the outside with a bath of H2O/ice.
The solution is slowly poured by regular drops and under agitation into 2000 ml of ethyl acetate. The precipitate is separated by filtration, washed 3 times with 100 ml of acetone/H2O 5:1 and 3 times with 100 ml of pure acetone, then vacuum dried.
Yield: 5.4 g.
b) To convert the carboxy salt of tetrabutylammo-nium residues in calcium salts, the procedure is as above, substituting the sodium chloride for calcium chloride.
Yield: 5.4 g.
Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

Example 15 - Preparation of the (partial) terbutYl ester of alqinic acid - 30% of the carboxy groups esterified -70% of the carboxy groups salified.
10 g (23.9 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained -from Laminaria hyPerborea) are solubilized in 400 ml of DMSO at 25 C. 1.34 g (7.18 m.Eq.) of terbutyl iodide are added.
The solution is well agitated for 12 hours at 30C.
a) For complete conversion of the carboxy salts of tetrabutylammonium residues to sodium salt, to the resulting solution is added 2.5 g of NaCl dissolved in 50 ml of distilled H2O, cooled from the outside with a bath o~f H2O/ice.
The solution is slowly poured by regular drops and under agitation into 2000 ml of ethyl acetate. The precipitate is separated by filtration, washed 3 times with 100 ml of acetone/H2O 5:1 and 3 times with 100 ml of pure acetone, then vacuum dried.
Yield: 5.5 g.
b) To convert the carboxy salt of tetrabutylammo-nium residues in calcium salts, the procedure is as above, substituting the sodium chloride for calcium chloride.
Yield: 5.7 g.
Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

Example 16 - PreParation of the (Partial) terbutyl ester of alginic acid - 10~ of the carboxy qroups esterified -90% of the carboxy groups salified.
10 g (23.9 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from , , . , ~i , -- 60 - 1 3 3 8 23 ~

Macrocystis PYrifera) are solubilized in 400 ml of DMSO
at 25C. 0.45 g (2.39 m.Eq.) of terbutyl iodide are added.
The solution is well agitated for 12 hours at 30 C.
a) For complete conversion of the carboxy salts of tetrabutylammonium residues to sodium salt, to the resulting solution is added 2.5 g of NaCl dissolved in 50 ml of distilled H2O, cooled from the outside with a bath of H2O/ice.
The solution is slowly poured by regular drops and under agitation into 2000 ml of ethyl acetate. The precipitate is separated by filtration, washed 3 times with 100 ml of acetone/H2O 5:1 and 3 times with 100 ml of pure acetone, then vacuum dried.
Yield: 5 g.
b) To convert the carboxy salt of tetrabutylammo-nium residues in calcium salts, the procedure is as above, substituting the sodium chloride for calcium chloride.
Yield: 5 g.
Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

Example 17 - Preparation of the (partial) benzyl ester of alqinic acid - 90% of the carboxy qroups esterified -10% of the carboxy qroups salified.
10 g (23.9 m.Eq.) of the tetrabutylzmmonium salt of ..
. ~ ~ .... . .

alginic acid (prepared from alginic acid obtained from AscoPh~llu.n nodosum) are solubilized in 400 ml of DMSO
at 25C. 3.76 g (21.5 m.Eq.) of benzyl bromide and 0.1 g of tetrabutylammonium iodide are added.
The solution is well agitated for 12 hours at 30C.
a) For complete conversion of the carboxy salts of tetrabutylammonium residues to sodium salt, to the resulting solution is added 2.5 g of NaCl dissolved in 50 ml of distilled H2O, cooled from the outside with a bath of H2O/ice.
The solution is slowly poured by regular drops and under agitation into 2000 ml of ethyl acetate. The precipitate is separated by filtration, washed 3 times with 100 ml of acetone/H2O 5:1 and 3 times with 100 ml of pure acetone, then vacuum dried.
Yield: 5 g.
b) To convert the carboxy salt of tetrabutylammo-nium residues in calcium salts, the procedure is as above, substituting the sodium chloride for calcium chloride.
Yield: 5 g.
Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

ExamPle 18 - Preparation of the (partial) benzyl ester of alqinic acid - 70% of the carboxy groups esterified -30% of the carboxy qrouPs salified.
10 g (23.9 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from Laminaria hyperborea) are solubilized in 400 ml of DMSO
at 25C. 2.9 g (16.7 m.Eq.) of benzyl bromide and 0.1 g of tetrabutylammonium iodide are added.
The solution is well agitated for 12 hours at 30C.
a) For complete conversion of the carboxy salts of tetrabutylammonium residues to sodium salt, to the resulting solution is added 2.5 g of NaCl dissolved in 50 ml of distilled H2O, cooled from the outside with a bath of H2O/ice.
The solution is slowly poured by regular drops and under agitation into 2000 ml of ethyl acetate. The precipitate is separated by filtration, washed 3 times with 100 ml of acetone/H2O 5:1 and 3 times with 100 ml of pure acetone, then vacuum dried.
Yield: 4.6 g.
b) To convert the carboxy salt of tetrabutylammo-nium residues in calcium salts, the procedure is as above, substituting the sodium chloride for calcium chloride.
Yield: 4.5 g.
Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

ExamPle 19 - Preparation of the (partial) benzYl ester of alginic acid - 50% of the carboxY qrouPs esterified -50% of the carboxy qrouPs salified.
10 g (23.9 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from Ascophyllum nodosum) are solubilized in 400 ml of DMSO
at 25C. 2.1 g (11.9 m.Eq.) of benzyl bromide and 0.1 g of tetrabutylammonium iodide are added.
The solution is well agitated for 12 hours at 30C.
a) For complete conversion of the carboxy salts of tetrabutylammonium residues to sodium salt, to the resulting solution is added 2.5 g of NaCl dissolved in 50 ml of distilled H2O, cooled from the outside with a bath of H2O/ice.
The solution is slowly poured by regular drops and under agitation into 2000 ml of ethyl acetate. The precipitate is separated by - filtration, washed 3 times with 100 ml of acetone/H2O 5:1 and 3 times with 100 ml of pure acetone, then vacuum dried.
Yield: 4.2 g.
b) To convert the carboxy salt of tetrabutylammo-nium residues in calcium salts, the procedure is as above, substituting the sodium chloride for calcium chloride.
Yield: 4.3 g.
Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

Example 20 - Preparation of the (Partial) benzYl ester of alginic acid - 30% of the carboxy qrouPs esterified -70% of the carboxy groups salified.
10 g (23.9 m.Eq.) of the tetrabutylammonium salt of ,. . ., , ' ; ,i D
'' ' . '' ' '.- , ..

alginic acid (prepared from alginic acid obtained from AscophYllum nodosum) are solubilized in 400 ml of DMSO
at 25C. 1.25 g (7.18 m.Eq.) of benzyl bromide and 0.1 g of tetrabutylammonium iodide are added.
The solution is well agitated for 12 hours at 30C.
a) For complete conversion of the carboxy salts of tetrabutylammonium residues to sodium salt, to the resulting solution is added 2.5 g of NaCl dissolved in 50 ml of distilled H2O, cooled from the outside with a bath of H2O/ice.
The solution is slowly poured by regular drops and under agitation into 2000 ml of ethyl acetate. The precipitate is separated by filtration, washed 3 times with 100 ml of acetone/H2O 5:1 and 3 times with 100 ml of pure acetone, then vacuum dried.
Yield: 6 g.
b) To convert the carboxy salt of tetrabutylammo-nium residues in calcium salts, the procedure is as above, substituting the sodium chloride for calcium chloride.
Yield: 6.1 g.
Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

Example 21 - Preparation of the (Partial) benzyl ester of alginic acid - 10% of the carboxy qrouPs esterified -90% of the carboxy qroups salified.
10 g (23.9 m.Eq.) of the tetrabutylammonium salt of ,~ :?.` -~

alginic acid (prepared from alginic acid obtained from MacrocYstis Pyrifera) are solubilized in 400 ml of DMSO
at 25C. 0.42 g (2.39 m.Eq.) of benzyl bromide and 0.1 g of tetrabutylammonium iodide are added.
The solution is well agitated for 12 hours at 30C.
a) For complete conversion of the carboxy salts of tetrabutylammonium residues to sodium salt, to the resulting solution is added 2.5 g of NaCl dissolved in 50 ml of distilled H2O, cooled from the outside with a bath of H2O/ice. The solution is slowly poured by regular drops being kept in agitation into 2000 ml of ethyl acetate.
The precipitate is separated by filtration, washed 3 times with 100 ml of acetone/H2O 5:1 and 3 times with 100 ml of pure acetone, then vacuum dried.
Yield: 5 g.
b) To convert the carboxy salt of tetrabutylammo-nium residues in calcium salts, the procedure is as above, substituting the sodium chloride for calcium chloride.
Yield: 5 g.
Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

ExamPIe 22 - Preparation of the methyl ester of alginic acid.
8.35 g (20 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from AscoPhYllum nodosum) are solubilized in 400 ml of DMSO
at 25C. 3.66 g (25 m.Eq.) of methyl iodide are added.
The solution is well agitated for 12 hours at 30C, and then slowly poured by regular drops and under agitation into 3.5 1 of ethyl acetate (or toluene). The precipitate is filtered and then washed 4 times with ethyl acetate and lastly vacuum dried for 24 hours at 30C. In this way 4 g of the compound named in the title are obtained.
Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

ExamPle 23 - Preparation of the benzYl ester of alqinic acid.
10 g (23.9 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from MacrocYstis pyrifera) are solubilized in 400 ml of DMSO
at 25C. 4.45 g (26 m.Eq.) of benzyl bromide and 0.1 g of tetrabutylammonium iodide are added.
The solution is well agitated for 12 hours at 30C, and then slowly poured by regular drops and under agitation into 3.5 1 of ethyl acetate (or toluene). The precipitate is filtered and then washed 4 times with ethyl acetate and lastly vacuum dried for 24 hours at 30C. In this way 5 g of the compound named in the title are obtained.

Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

Example 24 - Preparation of the terbutyl ester of alginic acid.
10 g (23.9 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from Laminaria hyperborea) are solubilized in 400 ml of DMSO
at 25C. 4.8 g (26 m.Eq.) of terbutyl iodide are added.
The solution is well agitated for 12 hours at 30C, and then slowly poured by regular drops and under agitation into 3.5 1 of ethyl acetate (or toluene). The precipitate is filtered and then washed 4 times with ethyl acetate and lastly vacuum dried for 24 hours at 30C. In this way 3.8 g of the compound named in the title are obtained.
Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

Example 25 - Preparation of the isopropyl ester of alqinic acid.
10 g (23,9 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from Laminaria hyperborea) are solubilized in 400 ml of DMSO

~, ;. . .

-at 25C. 4.4 g (26 m.Eq.) of isopropyl iodide are added.
The solution is well agitated for 12 hours at 30C, and then slowly poured by regular drops and under agitation into 3.5 1 of ethyl acetate (or toluene). The precipitate is filtered and then washed 4 times with ethyl acetate and lastly vacuum dried for 24 hours at 30C. In this way 4.5 g of the compound named in the title are obtained.
Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

Example 26 - Preparation of the ethyl ester of alqinic acid.
10 g (23.9 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from Ascophyllum nodosum) are solubilized in 400 ml of DMSO
at 25C. 4 g (26 m.Eq.) of ethyl iodide are added.
The solution is well agitated for 12 hours at 30C, and then slowly poured by regular drops and under agitation into 3.5 1 of ethyl acetate (or toluene). The precipitate is filtered and then washed 4 times with ethyl acetate and lastly vacuum dried for 24 hours at 30C. In this way 4.5 g of the compound named in the title are obtained.
Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

. ; ' ' , , .~ , .
; ' . , ' ' ~ ~ . . . ", ' , . . . ' :.

-69a - 1 33~3~

Example 26A - Preparation of the amikacin salt of alginic acid partially esterified with ethanol - 75% of carboxylic groups esterified with ethanol - 25% of carboxylic qroups salified with amikacin.
147 mg of amikacin (1 m.Eq.) are solubilized in 20 ml of water.
0.81 g of a 75% ethyl ester of alginic acid and sodium salt at 25% (corresponding to 1 m.Eq. of a monomeric unit relative to the non-esterified carboxyl), are solubilized in 400 ml of water. The solution is eluted in a thermostatic column at 20 and containing 2 ml of sulfonic resin (Dowex 50 x 8) in H+ form.
The sodium-free eluate is gathered under agitation in the solution of amikacin base. The resulting solution is instantly frozen and freeze-dried.
Microbiological determination carried out on St.
aureus ATCC 29737 in comparison to standard amikacin, shows a content of 8.5% in weight of amikacin base, corresponding to the theoretically calculated value.

Example 26B - Preparation of erythromycin salt of alqinic acid partially esterified with ethanol - 75% of carboxylic qroups esterified with ethanol - 25% of carboxylic qroups salified with erYthromycin.
0.81 g of a 75% ethyl ester of alginic acid and sodium salt at 25% (corresponding to 1 m.Eq. of a monomeric unit relative to the non-esterified carboxyl), are solubilized in 400 ml of water. The solution is eluted in a thermostatic column at 20 containing 2 ml of sulfonic resin (Dowex 50 x 8) in H+ form.

.. .: . . .
. -; . . .. . ,-..................... . ..

-69b - ~ 338235 To the sodium-free eluate are added 734 mg of erythromycin base (1 m.E.q.). The resulting solution is instantly frozen and freeze-dried.
Microbiological determination on St. aureus ATCC
6538 in comparison to standard erythromycin, shows a content of 31.7% in weight of erythromycin base, corresponding to the theoretically calculated weight.

Example 26C - PreParation of streptomycine salt of alginic acid partially esterified with ethanol - 75% of carboxylic groups esterified with ethanol - 25% of carboxylic qroups salified with streptomycine.
243 mg of streptomycine sulphate (1 m.Eq.) are solubilized in 20 ml of water. The solution of eluted in a thermostatic column at 5 containing 2 ml of quaternary ammonium resin (Dowex 1 x 8) in OH~form.
The sulphate-free eluate is gathered in a thermostatic container at a temperature of 5.
0.81 g of a 75% ethyl ester of alginic acid and 25%
sodium salt (corresponding to 1 m.Eq. of a monomeric unit relative to the non-esterified carboxyl), are solubilized in 400 ml of water. The solution is eluted in a thermostatic column at 20 and containing 2 ml of sulphonic resin (Dowex 50 x 8) in H+ form.
The sodium-free eluate is gathered under agitation in the solution of streptomycine base. The resulting solution is instantly frozen and freeze-dried.
Microbiological determination on B. subtilis ATCC
6633 in comparison with streptomycine standard, shows a content of 10.9% in weight of streptomycine base, corresponding to the theoretically calculated content.

. ~ , -69c - 1 3 3 8 2 3 5 Example 26D - PreParation of the (partial and mixed ethanol and fluorocortisone esters (C21) of alginic acid - 40% of carboxylic qroups esterified with ethanol - 20%
of carboxylic qroups esterified with fluorocortisone (C21) - 40% of salified carboxylic groups (Na).
8.35 g of the tetrabutylammonium salt of alginic acid (prepared from Laminaria hyperborea) corresponding to 20 m.Eq. of a monomeric unit are solubilized in 350 ml of dimethylsulfoxide at 25, 0.62 g (4 m.Eq.) of ethyl iodide are added and the solution is kept for 24 hours at 300.
0.89 g (2 m.Eq.) of 9C~-fluoro-21-bromo-4-pregnene-11~ , 17 ~ -diol-3, 20-dione are added and the solution is kept for 24 hours at 30.
A solution is then added containing 100 ml of water and 5 g of sodium chloride and the resulting mixture is slowly poured into 2,000 ml of acetone under constant agitation. A precipitate is formed which is filtered and washed three times with 100 ml of acetone/water 5:1 and three times with 100 ml acetone and finally vacuum dried for eight hours at 30.
3.5 g of the partial and mixed ethanol and fluorocortisone ester in the title are obtained.
Quantitative determination of fluorocortisone, after mild alkaline hydrolysis with hydroalcoholic solution of Na2C03 and extraction with chloroform, is carried out according to British Pharmacopea, 1980.
Quantitative determination of the ethoxyls is carried out according to R.H. Cundiff and P.C. Markunas [Anal. Chem. 33, 1028-1030 ~1961)].

w -69d ~ 1 338235 Example 26E - Preparation of the (partial) fluorocortisone esters (C21) of alginic acid - 20% of esterified carboxylic groups - 80% of salified carboxylic groups (Na).
4.18 g of the tetrabutylammonium salt of alginic acid (prepared from Laminaria hyperborea) corresponding to 10 m.Eq. of a monomeric unit are solubilized in 210 ml of dimethylsulfoxide at 25, 0.89 g (2 m.Eq.) of gc~
-fluoro-21-bromo-4-pregnene-11~ , 17~ -diol-3,20-dione are added and the resulting solution is kept for 12 hours at 30.
A solution is then added containing 62 ml of water and 5 g of sodium chloride and the resulting mixture is slowly poured into 2,000 ml of acetone under constant agitation. A precipitate is formed which is filtered and washed three times with 100 ml of acetone/water 5:1 and three times with acetone and finally vacuum dried for eight hours at 30.
The product is then dissolved in 300 ml of water containing 1% of sodium chloride and the solution is slowly poured into 1,500 ml of acetone under constant agitation. A precipitate is formed which is filtered and washed twice with 100 ml of acetone/water 5:1 and three times with 100 ml of acetone and finally vacuum dried for 24 hours at 30. 1.5 g of the partial fluorocortisone compound in the title are obtained.
Quantitative determination of fluorocortisone after mild alkaline hydrolysis with hydroalcoholic solution of Na2C03 and extraction with chloroform, is carried out according to British Pharmacopea, 1980, p. 196.

-69 e- 1 338235 Example 26F - PreParation of the (mixed) ethanol and hydrocortisone esters (C21~ of alqinic acid - 80% of carboxylic groups esterified with ethanol - 20% of carboxylic qroups esterified with hYdrocortisone (C211.
4.18 g of the tetrabutylammonium salt of alginic acid (prepared from Laminaria hyperborea) corresponding to 10 m.Eq. of a monomeric unit are solubilized in 210 ml of dimethylsulfoxide at 25, 1.25 g (8 m.Eq.) of ethyl iodide are added and the solution is kept at 30 for 12 hours.
0.85 g (2 m.Eq.) of 21-bromo-4-pregnene-11~ , 17~ -diol-3,20-dione are added and the solution is kept for 24 hours at 30.
A solution is then added containing 100 ml of water and 5 g of sodium chloride and the resulting mixture is slowly poured into 2,000 ml of acetone under constant agitation. A precipitate is formed which is filtered and washed three times with 100 ml of acetone/water 5:1 and three times with 100 ml of acetone and finally vacuum dried for eight hours at 30.
1.8 g of the mixed ethanol and hydrocortisone ester compound in the title are obtained. Quantitative determination of hydrocortisone, after mild alkaline hydrolysis with hydroalcoholic solution of Na2C03 and extraction with chloroform, is carried out according to British Pharmacopea, 1980.
Quantitative determination of the ethoxyls is carried out according to R.H. Cundiff and P.C. Markunas [Anal. Chem. 33, 1028-1030)].

:, . , "

-69f ~ 1 3 3 8 2 3 5 Example 26G - Preparation of the (partial) hydrocortisone esters (C21) of alqinic acid - 20% of esterified carbox~lic groups - 80% of salified carboxylic qrouPs fNa).
8.35 g of the tetrabutylammonium salt of alginic acid (prepared from Microcystis pyrifera) corresponding to 20 m.Eq. of a monomeric unit are solubilized in 350 ml of dimethylsulfoxide at 25, 0.850 g. (2 m.Eq.) of 21-bromo-4-pregnene~ , 17 ~-diol-3,20-dione are added and the resulting solution is kept for 24 hours at 30.
A solution is then added containing 100 ml of water and 5 g of sodium chloride and the resulting mixture is slowly poured into 2,000 ml of acetone under contant agitation. A precipitate is formed which is filtered and whashed three times with 100 ml of acetone/water 5:1 and three times with acetone and finally vacuum dried for eight hours at 30.
The product is then dissolved in 300 ml of water containing 1% of sodium chloride and the solution is slowly poured into 1,500 ml of acetone under constant agitation. A precipitate is formed which is filtered and washed twice with 100 ml of acetone/water 5:1 and three times with 100 ml of acetone and finally vacuum dried for 24 hours at 30.
3 g of the partial hydrocortisone compound in the title are obtained.
Quantitative determination of hydrocortisone after mild alkaline hydrolysis with hydroalcoholic solution of Na2C03 and extraction with chloroform, is carried out according to British Pharmacopea, 1980, p. 224.

-~69g - 1 3 3 8 ~ 3 5 Example 26H - Preparation of the (mixed) ethanol and fluorocortisone ester (C21) of alqinic acid - 80% of carboxylic qroups esterified with ethanol - 20% of carboxylic groups esterified with fluorocortisone (C21L.
4.18 g of the tetrabutylammonium salt of alginic acid (prepared from Macrocystis PYrifera) corresponding to 10 m.Eq. of a monomeric unit are solubilized in 210 ml of dimethylsulfoxide at 25, 1.25 g (8 m.Eq.) of ethyl iodide are added and the solution is kept for 24 hours at 3oo.
0.89 g (2 m.Eq.) of 9C~- fluoro-21-bromo-4-pregnene-11~ , 17~-diol-3,20-dione are added and the solution is kept for 24 hours at 30.
A solution is then added containing 100 ml of water and 5 g of sodium chloride and the resulting mixture is slowly poured into 2,000 ml of acetone under constant agitation. A precipitate is formed which is filtered and washed three times with 100 ml of acetone/water 5:1 and three times with 100 ml of acetone and finally vacuum dried for eight hours at 30.
1.7 g of the mixed ethanol and fluorocortisone ester compound featured in the title are obtained.
Quantitative determination of fluorocortisone, after mild alkaline hydrolysis with hydroalcoholic solution of Na2C03 and extraction with chloroform, is carried out according to British Pharmacopea, 1980.
Quantitative determination of the ethoxyls is carried out according to R.H. Cundiff and P.C. Markunas [Anal. Chem. 33, 1028-1030 (1961)].

-69h -Example 26I - PreParation of the (partial and mixed) ethanol and hydrocortisone ester (C21) of alginic acid -40% of carboxylic groups esterified with ethanol - 20% of carboxYlic groups esterified with hydrocortisone (C21) -40% of salified carboxylic groups (Na).
4.18 g of the tetrabutylammonium salt of alginic acid (prepared from Macrocystis pyrifera) corresponding to 10 m.Eq. of a monomeric unit are solubilized in 210 ml of dimethylsulfoxide at 25, 0.62 g (4 m.Eq.) of ethyl iodide are added and the solution is kept for 24 hours at 3oo.
0.85 g (2 m.Eq.) of 21-bromo-4-pregnene-11~ , 17~ -diol-3,20-dione are added and the solution is kept for 24 hours at 30.
A solution is then added containing 200 ml of water and 5 g of sodium chloride and the resulting mixture is slowly poured into 2,000 ml of acetone under constant agitation. A precipitate is formed which is filtered and washed three times with 100 ml of acetone/water 5:1 and three times with 100 ml of acetone and finally vacuum dried for eight hours at 30.
1.7 g of the partial and mixed ethanol and hydrocortisone ester compound in the title are obtained.
Quantitative determination of hydrocortisone, after mild alkaline hydrolysis with hydroalcoholic solution of Na2C03 and extraction with chloroform, is carried out according to British Pharmacopea, 1980.
Quantitative determination of the ethoxyls is carried out according to R.H. Cundiff and P.C. Markunas [Anal. Chem. 33, 1028-1030 (1961)].

,,. . . . ., ~" ,~ :

1 ~ 3 ~

_ 70 As noted hereinbefore, one object of`the invention provided by the heretofore-mentioned divisional application was the provision of pharmaceutical preparations containing one or more total, water-insoluble alginic acid esters as described above or medicaments resulting from association of one such total, water-insoluble ester with a pharmacologically-active substance as described above, that is, medicaments in which the total, water-insoluble alginic ester acts as a vehicle substance.
The pharmaceutical preparations containing thera-peutically-active total, water-insoluble alginic esters, possibly in the form of the above medicaments resulting from the association of components (1) and (2), contain the usual excipients and may be destined for oral, rectal, parenteral, subcutaneous, local or intradermal use. They are therefore in solid or semisolid form, for example pills, tablets, gelatin capsules, capsules, suppositories, soft gelatin capsules. For parenteral and subcutaneous use, it is possible to use forms intended for intramuscular and intradermal administration, or suitable for intravenous infusion or injections. It is therefore possible to present active compounds as solutions or as freeze-dried powders to unite with one or more excipients or diluents acceptable from a pharmaceutical point of view and convenient for the above uses and of compatible osmolarity with the physiological fluids. For local use, preparations in spray form should be considered, for example, nasal r~

~_ 71 sprays, creams or ointments for topical use or suitably prepared plasters for intradermal administration.
The preparation of the invention provided by the heretofore-mentioned divisional application may be intended for administration to man or animal. These contain prefer-ably between 0.01% and 10% of active component for the solutions, sprays, ointments and creams and between 1% and 100% and preferably between 5% and 50% of the active com-pound for the preparation in solid form. The dosage to be administered depends on the particular indication, and on the desired effect of chosen administration route. The daily dosage of these preparations may be estimated from those in use for the corresponding known preparations for the corresponding uses of the therapeutically-active alcohol, whose action is to be exploited. In this may, for example, the dosage of a total, water-insoluble alginic ester with cortisone may be derived from its content in this same steroid and from its usual dosage in the known pharmaceutical preparation.
One particular form of pharmaceutical preparations is represented by the above-described medicaments constituted by the association of a total, water-insoluble alginic ester and an active substance, for example, for topical use. These may also be in solid form, for example, as freeze-dried powders containing only the two components (1) and (2) as a mixture or separate. When these medicaments in solid form come into contact with the epithelium to be treated, they form more or less concentrated solutions _ 72 l 338235 according to the nature of the particular epithelium to be treated, with the same characteristics as the solutions previously prepared in vitro and which represent another particularly important aspect of the invention provided by the heretofore-mentioned divisional application. These solutions are preferably made with distilled water or sterile saline and preferably contain no other pharmaceutical vehlcle except the total, water-insoluble alginic ester or one of its salts.
The concentrations of these solutions may also vary greatly, for example, between 0.01 and 75% both for each of the two components considered separately, and for their mixture or salts. Preference is given in particular, to solutions with a pronounced elastic-viscous character, for example, with a content of between 10% and 90% of the medi-cament or of each of its components.
Of particular importance are medicaments of this type, both in anhydrous form (freeze-dried powders) or as concen-trated solutions or diluted in water or saline, possibly with the addition of additive or auxiliary substance, e.g., in particular disinfectant substances or mineral salts acting as buffers or others, used for ophthalmic purposes.
Of the medicaments of the invention provided by the heretofore-mentioned divisional application, those to be chosen, as the case may be, are those with a degree of acidity suitable for the zone to which they are to be applied, that is with a physiologically-tolerable pH.
Adjustment of the pH, for example in the above mentioned 1 33823~
_ 73 salts of the total, water-insoluble alginic acid esters with a basic active substance, may be effected by suitably regulating the quantities of polysaccharide, its salts and of the basic substance itself. In this way, for example, if the acidity of a total, water-insoluble alginic ester salt with a basic substance is too high, the excess of free acid groups can be neutralized with the above-mentioned inorganic bases, for example, with sodium, potassium or ammonium hydrate.
Preparation of the salts according to the invention provided by the heretofore-mentioned divisional application may be carried out in the known way, by bringing into con-tact solutions or aqueous suspensions or in organic sol-vents of the two components (1) and (2) and possibly of bases or basic salts of the above mentioned alkaline or alkaline earth metals or magnesium or aluminum in cal-culated quantities and isolating the salts in anhydrous amorphous form according to the known methods. It is possible, for example, first of all to prepare aqueous solutions of the two components (1) and (2), freeing these components from aqueous solutions of their salts with suitable ion-exchangers, uniting the two solutions at a low temperature, for example, between 0 and 20C, if the salts thus obtained are easily soluble in water it is freeze-dried, while salts with poor solubility can be separated bycentrifugation or filtration or decantation and possibly subsequently dried.

_ . 74 l 338235 For these associated medicaments too, the dose is based on that of the active principles used singly and may therefore be easily determined by those skilled in the art, considering the doses recommended for the corresponding known medicaments.
In the cosmetic articles according to the invention provided by the heretofore-mentioned divisional applica-tion, the total, water-insoluble alginic esters and their salts are mixed with the excipients commonly used in this field and are, for example, those already listed above for the pharmaceutical preparation. Above all, creams, ointments, lotions may be used for topical use in which the total, water-insoluble alginic ester or one of its salts may constitute the active cosmetic principle possibly with the addition of other cosmetically active principles, e.g., steroids, for example pregnenolone, or one of the prin-ciples previously reported. In these preparations, the total, water-insoluble alginic ester may be an ester with a cosmetically active alcohol, e.g., dexpanthenol, or also an ester with an alcohol having no cosmetic action, e.g., lower aliphatic alcohol, for example, one of those already quoted: the effect is due to the intrinsic cosmetic proper-ties of the polysaccharide component, e.g., in the case of free alginic acid or of its salts.
The cosmetic articles may however, be used on various other active principles, for example disinfectant sub-stances, sun shields, water-repellents, regenerating or antiwrinkle substances, or odoriferous substances, espe-G

_ 75 1338235 cially perfumes. In this case, the total, water-insoluble alginic ester itself may be the active ingredient and may derive from alcohols with these same properties, for example, from higher aliphatic alcohols or terpene alcohols in the case of perfumes, or act above all as a vehicling substance, for instance, with those properties which are associated with it. Particularly important therefore are cosmetic composi-tions similar to the medicaments described above in which the pharmaceutically-active component (1) is substituted by a cosmetological factor, and the respective salts. Use of the above esters deriving from alcohols used in the perfume industry represents a great step ahead in the advance of technique, since it allows a slow, constant and protracted release of the odoriferous principles.
The following are particular exemplary pharmaceutical preparations according to the invention provided by the heretofore-mentioned divisional application.
Formulation 1 - Collirium containing cortisone of 20 which 100 ml contain:
- partial ester of alginic acid with cortisone, g.
0.200 - ethyl p. hydroxybenzoate, gr. 0.010 - methyl p. hydroxybenzoate, gr. 0.050 - sodium chloride, gr. 0.0900 - water for injectable preparations/q.b.a., ml. 100 Formulation 2 - Injectable solution containing hydrocortisone of which 100 ml contain:

G

' 76 - partial ester of alginic acid with hydrocortisone, gr. 0.1 - water for injectable preparations/g.b.a., ml 100 Formulation 3 - Cream containing a partial ester of alginic acid with ethyl alcohol, of which 100 gr. contain:
- partial ester of alginic acid with ethyl alcohol, ~ r. 0.2 - ~Polyethylene glycol monostearate 400, gr. 10.000 - CETIOL V (Trade-mark), gr. 5.000 - LENETTE SX (Trade-mark for an emulsifying wax), gr. 2.000 - Paraoxybenzoate of methyl, gr. 0.07S
- Paraoxybenzoate of propyl, gr. 0.050 - Sodium dihydroacetate, gr. 0.100 - Glycerine F.U., gr. 1.500 - Sorbitol 70, gr. 1.500 - Test cream, gr. 0.050 - Water for injectable preparations/q.b.a., gr.
100 . 00 One important application of aspects of the present invention regards the sanitary and surgical articles already described, the methods for their manufacture and their use. The invention therefore includes all the articles similar to those already on the market made with alginic acid but containing a total, water-insoluble alginic ester or one of its salts in place of the free acid or one of its salts.

C~

_ 77 l 338235 Completely new surgical and sanitary articles according to aspects of the present invention are repre-sented by the total, water-insoluble esters of alginic acid regenerated as such from appropriate organic solutions and capable of being made into sheet and thread form, thus obtaining films, sheets and threads for use in surgery, as skin auxiliaries and substitutes in cases of serious damage to this organ, e.g., following burns, or as suture threads in surgical operations. The present invention, in another of its aspects, includes, in particular, these uses and a preparation procedure for such articles consisting in the formation of a solution of the total, water-insoluble alginic ester or of one of its salts in an appropriate organic solvent, for example, a ketone, an ester or an aprotic solvent, e.g., an amide of a carboxylic acid, especially a dialkylamide or of an aliphatic acid with between 1 and 5 carbon atoms and deriving from alkyl groups with between 1 and 6 carbon atoms, particularly by an organic sulfoxide, that is a dialkylsulfoxide with alkyl groups with a maximum of 6 carbon atoms, e.g., especially dimethylsulfoxide or diethylsulfoxide and, most preferably, a fluorurate solvent with a low boiling point, e.g. espe-cially hexafluoroisopropanol.
An aspect of the present invention then consists in making these solutions into sheets or threads and in removing the organic solvent by contact with a second organic or aqueous solvent, capable of being mixed with the first solvent and in which the total, water-insoluble _ ~ 78 l 338235 alginic ester is not soluble, especially a lower aliphatic alcohol, for example ethyl alcohol (for wet spinning), or should a solvent with a fairly low boiling point have been used to prepare the solutions of the total, water-insoluble alginic esters, removing such solvent under dryconditions with a current of gas, and especially suitably heated nitrogen (e.g., dry spinning). Excellent results can also be obtained with combination dry-wet spinning.
The threads obtained with the total, water-insoluble alginic acid esters may be used for the preparation of gauzes to be used for the medication of wounds and in surgery. The gauzes have the exceptional advantage of biodegradability in the organism, made possible by the naturally-existing enzymes. These enzymes divide the total, water-insoluble ester into alginic acid and the corresponding alcohol, when a total, water-insoluble alginic ester deriving from a therapeutically-acceptable alcohol is used, e.g., ethyl alcohol.
These gauzes and also the above-described threads may therefore also be left inside the organism after surgery, being then slowly absorbed after the previously mentioned process of degradation.
In the preparation of the above-described sanitary and surgical articles of aspects of this invention, it is con-venient to add conventional plasticizing materials in orderto improve their mechanical characteristics, e.g., as in the case of threads to improve their resistance to knots G

and tangles. Such plasticizers may, for example, be alkaline salts of fatty acids, for example, sodium stearate or sodium palmitate, the total, water-insoluble esters of organic acids with a high number of carbon atoms, etc.
Another application of the new total, water-insoluble esters is represented by the preparation of capsules for subcutaneous implantation of medicaments or of micro-capsules for injection, for example by subcutaneous or intramuscular route, where their biodegradability is exploited by the esterases present in the organism.
Of great importance also is the preparation of micro-capsules made with total, water-insoluble alginic esters, solving the problem previously connected with their use, up till now very limited, for the same reasons as those set out previously, opening up a wide field of application where a "retard" effect is desired after administration by injection.
A further application of the new total, water-insolu-ble esters in the field of medicine and surgery involves the preparation of a wide variety of solid inserts, e.g., plates, discs, laminas, etc. substituting for those made of metal or synthetic plastic material already in use, in cases where such inserts are to be removed after a certain period of time. Preparations based on animal collagens, being of a proteinaceous nature, often give rise to unplea-sant reactions, e.g. inflammation or rejection symptoms.
In the case of total, water-insoluble alginic esters, this danger does not exist.

79a Part of the applications in the medical-surgical field according to the aspects of present invention using these new total, water-insoluble esters concerns preparations using expansile materials, especially in the forms of sponges, for the medication of wounds or various types of lesion.
The following preparations exemplify the medical articles according to aspects of the invention containing the total, water-insoluble alginic esters.
Example 27 - Preparation of films usinq esters of alginic acid.
A solution is prepared in dimethylsulfoxide of the n-propyl ester of alginic acid with a concentration of 180 mg/ml.
By means of a stratifier, a thin layer of solution is spread on a glass sheet; the thickness must be 10 times greater than the final thickness of the film. The glass is immersed in ethanol which absorbs the dimethylsulfoxide but does not solubilize the HY ester which becomes solid. The film is detached from the glass sheet, is repeatedly washed with ethanol, then with water and then again with ethanol.
The resulting sheet is dried in a press for 48 hours at 30.

G

Example 28 - Preparation of threads using esters of alginic acid.
A solution is prepared in dimethylsulfoxide of the benzyl ester of alginic acid with a concentration of 200 mg/ml. The solution thus obtained is pressed by means of a pump through a threader with 0.5 mm holes.
The threader is immersed in ethanol/dimethyl-sulfoxide 80:20 (this concentration is kept constant by continuous addition of ethanol); when the solution in dimethylsulfoxide is soaked in this way it tends to lose most of the dimethylsulfoxide and the thread solidifies.
The thread is stretched while it still has a content of dimethylsulfoxide, is then repeatedly stretched and washed with ethanol. The thread is dried in nitrogen current.

Example 29 - Preparation of a spongy material made with alginic esters.
1 g of benzyl ester of alginic acid in which all the carboxylic groups are esterified (obtained for example as described in Example 23) are dissolved in 5 ml of dimethylsulfoxide. To each 10 ml of solution prepared, a mixture of 31.S g of sodium chloride with a degree of granularity corresponding to 300~, 1.28 g of sodium bicarbonate and 1 g of citric acid is added and the whole is homogenized in a mixer.
The pasty mixture is stratified in various ways, for instance by means of a mange consisting of two rollers which turn opposite each other at an adjustable distance between the two. Regulating this distance the paste is -:

- 81 - ~ 3 3 ~ 2 3 ~

passed between the rollers together with a strip of silicone paper which acts as a support to the layer of paste thus formed. The layer is cut to the desired dimensions of length and breadth, removed from the silicone, wrapped in filter paper and emerged in a suitable solvent, such as water. The sponges thus obtained are washed with a suitable solvent such as water and possibly sterilized with gamma rays.

Example 30 - Preparation of a sPonqy material made with alginic acid esters.
In the manner described in Example 29, it is possible to prepare spongy materials with other alginic acid esters. In the place of dimethylsulfoxide it is possible to use, if desired, any other solvent capable of dissolving the chosen ester. In the place of sodium chloride it is possible to use any other solid compound which is insoluble in the solvent used to dissolve the hyaluronic acid ester, but which is however soluble in the solvent used to precipiate the hyaluronic ester after the above mentioned mechanical treatment, and finally which has the correct degree of granularity to obtain the type of pores desired in the sponge material.
In the place of sodium bicarbonate and citric acid it is possible to use other couples of similar compounds, that is, compounds which react to each other in suspension or solution of the solvent used to dissolve alginic acid in such a way as to form a gas, such as carbon dioxide, which has the effect of producing a less compact spongy material. In this way ~ 82 1 338235 it is possible to use, in the place of sodium bicarbonate, other bicarbonates or alkali metal or alkaline earth car-bonates and in place of citric acid, to use other acids in solid form, e.g., tartaric acid.

~,.

SUPPLEMENTARY DISCLOSURE

The Principal Disclosure provided total water-insoluble sanitary or surgical articles comprising, as an essential component, at least one total, water-insoluble ester of alginic acid with an alcohol selected from the group consisting of aliphatic, araliphatic, cycloaliphatic, aliphatic-cycloaliphatic and heterocyclic alcoholsl as well as possibly any incidental ingredients which may have been used heretofore in sanitary or surgical articles, e.g., where the alcohol was a) an aliphatic radical with a maximum of 34 carbon atoms; b) an araliphatic radical with only one benzene ring, and in which the aliphatic chain has a maximum of 4 carbon atoms; c) a cycloaliphatic radical which is mono- or polycyclic with a maximum of 34 carbon atoms; d) an aliphatic-cycloaliphatic radical which is mono- or polycyclic with a maximum of 34 carbon atoms; or e) a heterocyclic radical with a maximum of 34 carbon atoms in which the hetero atoms are selected from the group consisting of oxygen, sulfur and nitrogen, e.g. wherein a) the aliphatic, cycloaliphatic, aliphatic-cycloaliphatic and heterocyclic radicals are substituted by one or two func-tional groups selected from the group consisting of amino, hydroxy, mercapto, aldehyde, keto, carboxyl, hydrocarbyl, dihydrocarbylamino, ether, ester, thioether, thioester, acetal, ketal, carbalkoxy and carbamidic groups and carbamidic groups substituted by one or two alkyl groups, the hydrocarbyl radicals in these functional groups having G

SD 84 1 33823~
a ~;~um of 6 carbon atoms; or e.g. wherein the ester is the total, water-insoluble tert-butyl ester of alginic acid; e.g. wherein the aliphatic radical is derived from a member selected from the group consisting of methyl alcohol, ethyl alcohol, propyl alcohol, isopropyl alcohol, n-butyl alcohol, isobutyl alcohol, tert-butyl alcohol, amyl alcohol, pentyl alcohol, hexyl alcohol, octyl alcohols glycerin, tartronic alcohol, lactic acids, glycolic acid, malic acid, tartaric acid, citric acid, aminoethanol, aminopropanol, n-aminobutanol or their dimethyl or diethyl derivatives in the amino moiety, choline, pyrrolidinyl-ethanol, piperidinylethanol, piperazinylethanol, piper-azinyl-n-propyl alcohol, piperazinyl-n-butyl alcohol, monothioethylene glycol, myricyl alcohol, citronellol, géraniol, nerol, nerolidol, linalool, farnesol and phytol.
Specific examples of such total, water-insoluble esters were methyl, ethyl, isopropyl, tert-butyl, and benzyl.
These sanitary or surgical articles were taught as being in the form of a film or thread.
The Principal Disclosure also provided a procedure for the preparation of sanitary or surgical articles in the form of films or threads, the essential component of which comprised at least one total, water-insoluble ester of alginic acid with an alcohol selected from the group con-sisting of aliphatic, araliphatic, cycloaliphatic, ali-phatic-cycloaliphatic and heterocyclic alcohols, which ~' procedure comprised: dissolving the total, water-insoluble alginic ester in a first organic solvent; making the solution into sheet form or into thread form, respectively;
then eliminating the first organic solvent by treatment with a second suitable organic or with an aqueous solvent which is soluble in the first solvent; and then removing the second organic or aqueous solvent.
The purpose of the present Supplementary Disclosure is to provide sanitary or surgical articles comprising at least one further total, water-insoluble ester of alginic acid with a wide variety of alcohols; to provide additional procedures for preparing articles and to provide uses of such articles.
Accordingly, the present invention, as now provided by the present Supplementary Disclosure, provides as a broad aspect thereof, sanitary or surgical articles the essential component of which comprises at least one total, water-insoluble ester of alginic acid with an alcohol which is selected from the group consisting of cyclohexyl, sec-butyl, cyclobutyl, decyl, dodecyl, 2-phenylethyl, heptyl, hexyl, propyl, n-octyl, 2,6-dichlorobenzyl, 4-tert-butylbenzyl, heptadecyl, octadecyl, 3-phenylpropyl, 3,4,5-trimethoxybenzyl, cinnamyl, nonyl, n-pentylic, isopentylic, a mixture of ethyl and prednisolonyl alcohols, a mixture of ethyl and dexamethasonyl alcohols, a mixture of ethyl and cortisonyl alcohols, a mixture of ethyl and hydrocortisonyl alcohols, and a mixture of ethyl and desoxycorticosteronyl alcohols, as well as possibly any incidental ingredients ~c which may have been used heretofore in sanitary or surgical articles.
In one variant thereof, the alcohol may be selected from the group consisting of cyclohexyl, sec-butyl, cyclo-butyl, decyl, dodecyl, 2-phenylethyl, heptyl, hexyl, propyl, n-octyl, 2,6-dichlorobenzyl, 4-tert-butylbenzyl, heptadecyl, octadecyl, 3-phenylpropyl, 3,4,5-trimethoxy-benzyl, cinnamyl, nonyl, n-pentylic, and isopentylic.
In another variant thereof, the alcohol may be selected from the groups consisting of a mixture of ethyl and prednisolonyl alcohols, a mixture of ethyl and dexamethasonyl alcohols, a mixture of ethyl and cortisonyl alcohols, a mixture of ethyl and hydrocortisonyl alcohols, and a mixture of ethyl and desoxycorticosteronyl alcohols.
In yet another variant thereof, the alcohol may be selected from the group consisting of the (mixed) ethanolic and prednisolonic esters (C2l) of alginic acid - 80% of carboxylic groups esterified with ethanol - 20% of carboxy-lic groups esterified with prednisolone (C21); the (mixed)ethanolic and dexamethasonic esters (C2~) of alginic acid -80% of carboxylic groups esterified with ethanol - 20% of carboxylic groups esterified with dexamethasone (C21); the (mixed) ethanolic and cortisonic esters (C2l) of alginic acid - 80% of carboxylic groups esterified with ethanol -20% of carboxylic groups esterified with cortisone (C21);
the (mixed) ethanolic and hydrocortisonic esters (C2~) of alginic acid - 80% of carboxylic groups esterified with SD 87 1 33~3~
ethanol - 20% of carboxylic groups esterified with hydro-cortisone (C2l); and the (mixed) ethanolic and desoxycor-ticosteronic esters (C2l) of alginic acid - 80% of carboxylic groups esterified with ethanol - 20% of carboxylic groups esterified with desoxycorticosterone (C21) -By variants thereof, these articles may be in the form of a thread, or an artificial skin.
By another aspect of the present invention, as now provided by the present Supplementary Disclosure, a procedure is provided for the preparation of sanitary or surgical articles in the form of films or threads, the essential component of which comprises at least one total, water-insoluble ester of alginic acid with an alcohol selected from the group consisting of cyclohexyl, sec-butyl, cyclobutyl, decyl, dodecyl, 2-phenylethyl, heptyl, hexyl, propyl, n-octyl, 2,6-dichlorobenzyl, 4-terbutyl-benzyl, heptadecyl, octadecyl, 3-phenylpropyl, 3,4,5-tri-methoxybenzyl, cinnamyl, nonyl, n-pentylic, isopentylic, a mixture of ethyl and prednisolonyl alcohols, a mixture of ethyl and dexamethasonyl alcohols, a mixture of ethyl and cortisonyl alcohols, a mixture of ethyl and hydrocortisonyl alcohols, and a mixture of ethyl and desoxycorticosteronyl alcohols, which procedure comprises: dissolving the total, water-insoluble alginic ester in a first organic solvent;
making the solution into sheet or thread form respectively;
then eliminating the first organic solvent by treatment SD 88 1 33~23~
with a second suitable organic or with an aqueous solvent which is soluble in thefirst solvent; and then removing the second organic or aqueous solvent.
By one variant thereof, the alcohol is selected from the groups consisting of cyclohexyl, sec-butyl, cyclobutyl, decyl, dodecyl, 2-phenylethyl, heptyl, hexyl, propyl, n-octyl, 2,6-dichlorobenzyl, 4-tert-butylbenzyl, heptadecyl, octadecyl, 3-phenylpropyl, 3,4,5-trimethoxybenzyl, cinnamyl, nonyl, n-pentylic, and isopentylic.
By another variant thereof, the alcohol is selected from the group consisting of a mixture of ethyl and predni-solonyl alcohols, a mixture of ethyl and dexamethasonyl alcohols, a mixture of ethyl and cortisonyl alcohols, a mixture of ethyl and hydrocortisonyl alcohols, and a mixture of ethyl and desoxycorticosteronyl alcohols.
By yet another variant thereof the alcohol is selected from the group consisting of the (mixed) ethanolic and prednisolonic esters (C21) of alginic acid - 80% of carboxylic groups esterified with ethanol - 20% of carboxy-lic groups esterified with prednisolone (C21); the (mixed) ethanolic and dexamethasonic esters (C2l) of alginic acid -80% of carboxylic groups esterified with ethanol - 20% of carboxylic groups esterified with dexamethasone (C21); the (mixed) ethanolic and cortisonic esters (C2~) of alginic acid - 80% of carboxylic groups esterified with ethanol -20% of carboxylic groups esterified with cortisone (C21);
the (mixed) ethanolic and hydrocortisonic esters (C2~) of alginic acid - 80% of carboxylic groups esterified with 1 3382~5 ethanol - 20% of carboxylic groups esterified with hydro-cortisone (C2l); and the (mixed) ethanolic and desoxycorti-costeronic esters (C2l) of alginic acid - 80~ of carboxylic groups esterified with ethanol - 20% of carboxylic groups esterified with desoxycorticosterone (C2~).
The present invention, as now provided by the present Supplementary Disclosure, also provides a method of using the above-described threads, the essential component of which comprises the total, water-insoluble alginic acid esters as suture threads, e.g. by dissolving the total, water-insoluble alginic ester in a first organic solvent;
making the solution into thread form; then eliminating the first organic solvent by treatment with a second suitable organic or with an aqueous solvent which is soluble in the first solvent; then removing the second organic or aqueous solvent; and then using the threads as well as possibly any incidental ingredients which may have been used heretofore as suture threads in surgical articles in surgical operations.
By one variant thereof, the alcohol is selected from the groups consisting of cyclohexyl, sec-butyl, cyclobutyl, decyl, dodecyl, 2-phenylethyl, heptyl, hexyl, propyl, n-octyl, 2,6-dichlorobenzyl, 4-tert-butylbenzyl, heptadecyl, octadecyl, 3-phenylpropyl, 3,4,5-trimethoxybenzyl, cinnamyl, nonyl, n-pentylic, and isopentylic.
By another variant thereof, the alcohol is selected from the group consisting of a mixture of ethyl and predni-solonyl alcohols, a mixture of ethyl and dexamethasonyl SD go 1 338235 alcohols, a mixture of ethyl and cortisonyl alcohols, a mixture of ethyl and hydrocortisonyl alcohols, and a mixture of ethyl and desoxycorticosteronyl alcohols.
By yet another variant, the alcohol is selected from the group consisting of especially the (mixed) ethanolic and prednisolonic esters (C2l) of alginic acid - 80% of carboxylic groups esterified with ethanol - 20% of carboxy-lic groups esterifled with prednisolone (C21); the (mixed) ethanolic and dexamethasonic esters (C2l) of alginic acid -80% of carboxylic groups esterified with ethanol - 20% of carboxylic groups esterified with dexamethasone (C2~); the (mixed) ethanolic and cortisonic esters (C2l) of alginic acid - 80% of carboxylic groups esterified with ethanol -20% of carboxylic groups esterified with cortisone (C2l);
the (mixed) ethanolic and hydrocortisonic esters (C2l) of alginic acid - 80% of carboxylic groups esterified with ethanol - 20% of carboxylic groups esterified with hydro-cortisone (C2l); and the (mixed) ethanolic and desoxycorti-costeronic esters (C2~-) of alginic acid - 80% of carboxylic groups esterified with ethanol - 20% of carboxylic groups esterified with desoxycorticosterone (C2l).
G

~ SD 91 The present invention, as now provided by the present Supplementary Disclosure, also provides a method of using the above-described films, the essential component of which comprises the total, water-insoluble alginic acid esters as artificial skin, e.g. by dissolving the total, water-insoluble alginic ester in a first organic solvent; making the solution into sheet form; then eliminating the first organic solvent by treatment with a second suitable organic or with an aqueous solvent which is soluble in the first solvent; then removing the second organic or aqueous solvent; and then using the film as well as possibly any incidental ingredients which may have been used heretofore in surgical articles as artificial skin.
In one variant thereof, the alcohol is selected from the group consisting of cyclohexyl, sec-butyl, cyclobutyl, decyl, dodecyl, 2-phenylethyl, heptyl, hexyl, propyl, n-octyl, 2,6-dichlorobenzyl, 4-tert-butylbenzyl, heptadecyl, octadecyl, 3-phenylpropyl, 3,4,5-trimethoxybenzyl, cinnamyl, nonyl, n-pentylic, and isopentylic.
In another variant thereof, the alcohol is selected from the group consisting of a mixture of ethyl and predni-solonyl alcohols, a mixture of ethyl and dexamethasonyl alcohols, a mixture of ethyl and cortisonyl alcohols, a mixture of ethyl and hydrocortisonyl alcohols, and a mixture of ethyl and desoxycorticosteronyl alcohols.

~ SD 92 1 33~35 In yet another variant thereof, the alcohol is selected from the group consisting of the (mixed) ethanolic and prednisolonic esters (C2l) of alginic acid - 80% of carboxylic groups esterified with ethanol - 20% of carboxy-lic groups esterified with prednisolone (C2l); the (mixed) ethanolic and dexamethasonic esters (C2l) of alginic acid -80% of carboxylic groups esterified with ethanol - 20% of carboxylic groups esterified with dexamethasone (C21); the (mixed) ethanolic and cortisonic esters (C2l) of alginic acid - 80% of carboxylic groups esterified with ethanol -20% of carboxylic groups esterified with cortisone (C21);
the (mixed) ethanolic and hydrocortisonic esters (C21) of alginic acid - 80% of carboxylic groups esterified with ethanol - 20% of carboxylic groups esterified with hydro-cortisone (C21); and the (mixed) ethanolic and desoxycorti-costeronic esters (C2l) of alginic acid - 80% of carboxylic groups esterified with ethanol - 20% of carboxylic groups esterified with desoxycorticosterone (C2l).
The following are further examples of the present invention as now provided by the Supplementary Disclosure, i.e., to provide a method for the use of such thread as suture thread in surgical operations, or a method for using such film as artificial skin.

C~

- SD 93 1 33~23~

Example 31 - PreParation of the cyclohexyl ester of alqinic acid 10 g (23.9 m. Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from Laminaria hYper borea) are solubilized in 400 ml of DMS0 at 25C.
5.5g (26 m.Eq.) of Iodocyclohexane are added.

.
The solution is well agitated for 12 hours at 30C, and then slowly poured by regular drops and under agitation into 2.5 1 of ethyl acetate (or toluene). The precipitate is filtered and then washed 4 times with ethyl acetate and lastly vacuum dried for 24 hours at 30C. In this way 3 g of the compound named in the title are obtained.

Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

The degree of esterification is at least 99%.

SD 94 ~ 33~23~

Example 32 - PreParation of the sec-butYl ester of alginic acid 10 g (23.9 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from Laminaria hyper-borea) are solubilized in 400 ml of DMSO at 25C.
4.8 g (26 m.Eq.) of 2-Iodobutane are added.

The solution is well agitated for 12 hours at 30C, and then slowly poured by regular drops and under agitation into 3.5 1 of ethyl acetate (or toluene). The precipitate is filtered and then washed 4 times with ethyl acetate and lastly vacuum dried for 24 hours at 30C. In this way 3.5 g of the compound named in the title are obtained.

Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

The degree of esterification is at least 99%.

Example 331_ Preparation of the cYclobutYl ester of alginic ~cid 8.35 g (20 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from AscoPhYllum nodosum) are solubilized in 400 ml of DMS0 at 25C.
3.4 g (25 m.Eq.) of Bromocyclobutane are added.

The solution is well agitated for 12 hours at 30C, and then slowly poured by regular drops and under agitation into 3.5 l of ethyl acetate (or toluene). The precipitate is filtered and then washed 4 times with ethyl acetate and lastly vacuum dried for 24 hours at 30C. In this way 4 g of the compound named in the title are obtained.

Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

-The degree of esterification is at least 99%.

-- SD 96 1 33823~

Example 34 - Preparation of ~he Decyl ester of al~inic acid 8.35 g (20 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from Ascophyllum nodosum) are solubilized in 400 ml of DMS0 at 25C.
5.54 g (25 m.Eq.) of l-Bromodecane are added.

The solution is well agitated for 12 hours at 30C, and then slowly poured by regular drops and under agitation into 3.5 l of ethyl acetate (or toluene). The precipitate is filtered and then washed 4 times with ethyl acetate and lastly vacuum dried for 24 hours at 30C. In this way 4 g of the compound named in the title are obtained.

Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

- The degree of esterification is at least 99%.

`- 1 3~823~

Example 35 - Preparation of the DodecYl ester of alqinic acid 8.3S g (20 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from Asco~hyllum nodosum) are solubilized in 400 ml of DMSO at 25C.
6.23 g (25 m.Eq.) of 1-Bromododecane are added.

The solution is well agitated for 12 hours at 30C, and then slowly poured by regular drops and under agitation into 3.5 1 of ethyl acetate (or toluene). The precipitate is filtered and then washed 4 times with ethyl acetate and lastly vacuum dried for 24 hours at 30C. In this way, 4 g of the compound named in the title, are obtained.

Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

The degree of esterification is at least 99%.

~D

Example 36 - Preparation of the 2-Phenylethyl ester of al~inic acid 10 g (23.9 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from Macrocystis pyrifera) are solubilized in 400 ml of DMSO at 25C.
4.8 g (26 m.Eq.) of 2-Phenylethylbromide and 0.1 g of tetrabutyl-ammonium iodide are added.

The solution is well agitated for 12 hours at 30C, and then slowly poured by regular drops and under agitation into 3.5 1 of ethyl acetate (or toluene). The precipitate is filtered and then washed 4 times with ethyl acetate and lastly vacuum dried for 24 hours at 30C. In this way 5 g of the compound named in the title are obtained.

Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

The degree of esterification is at least 99%.

B~

Example 37 - Preparation of the HePtyl ester of al~inic acid 10 g (23.9 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from MacrocYstis pyrifera) are solubilized in 400 ml of DMSO at 25C.
5 g (28 m.Eq.) of Heptyl bromide and 0.1 g of tetrabutylammonium iodide are added.

The solution is well agitated for 12 hours at 30C, and then slowly poured by regular drops and under agitation into 3.5 1 of ethyl acetate (or toluene). The precipitate is filtered and then washed 4 times with ethyl acetate and lastly vacuum dried for 24 hours at 30C. In this way 4.5 g of the compound named in the title are obtained.

Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

The degree of esterification is at least 99%.

Example 38- PreParation of the He~l ester of alginic acid 10 g (23.9 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from Macrocystis pYrifera) are solubilized in 400 ml of DMSO at 25C.
4.3 g (26 m.Eq.) of Hexyl bromide and 0.1 g of tetrabutylammonium iodide are added.

The solution is well agitated for 12 hours at 30C, and then slowly poured by regular drops and under agitation into 3.5 l of ethyl acetate (or toluene). The precipitate is filtered and then washed 4 times with ethyl acetate and lastly vacuum dried for 24 hours at 30C. In this way 4 g of the compound named in the title are obtained.

Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

The degree of esterification is at least 99%.

1 33823~

Example 39 - PreParation of the ProDyl ester of alqinic acid 10 g (23.9 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from Asco~hyllum nodosum) are solubilized in 400 ml of DMSO at 25C.
4.4 g (26 m.Eq.) of Propyl iodide are added.

The solution is well agitated for 12 hours at 30C, and then slowly poured by regular drops and under agitation into 3.5 1 of ethyl acetate (or toluene). The precipitate is filtered and then washed 4 times with ethyl acetate and lastly vacuum dried for 24 hours at 30C. In this way 4.5 g of the compound named in the title are obtained.

Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

-The degree of esterification is at least 99%.

- , . . .

Example 40 - Preparation of the n-octyl ester of ~lqinic acid 8.35 g (20 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from AscoPhyllum nodosum) are solubilized in 400 ml of DMS0 at 25C.
4.83 g (25 m.Eq.) of l-bromo octane are added.

The solution is well agitated for 12 hours at 30C, and then slowly poured by regular drops and under agitation into 3.5 1 of ethyl acetate (or toluene). The precipitate is filtered and then washed 4 times with ethyl acetate and lastly vacuum dried for 24 hours at 30C. In this way 3.4 g of the compound named in the title are obtained.

Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

- The degree of esterification is at least 99%.

- ~ SD 103 Example 41 - PreParation of the 2,6-dichlorobenzyl e~ter of al~inic acid 8.35 g (20 m.E~.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from Asco~hvllum nodosum) are solubilized in 400 ml of DMS0 at 25C.
5.99 g (25 m.Eq.) of 2,6-dichlorobenzyl bromide are added.

The solution is well agitated for 12 hours at 30C, and then slowly poured by regular drops and under agitation into 3.5 1 of ethyl acetate (or toluene). The precipitate is filtered and then washed 4 times with ethyl acetate and lastly vacuum dried for 24 hours at 30C. In this way 3.8 g of the compound named in the title are obtained.

Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

The degree of esterification is at least 99%.

Example 42 - PreParation of the 4-terbutYlbenzyl ester of al~inic acid 8.35 g (20 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from AscophYllum nodosum) are solubilized in 400 ml of DMS0 at 25C.
5.67 g (25 m.Eq.) of 4-terbutylbenzyl bromide are added.

The solution is well agitated for 12 hours at 30C, and then slowly poured by regular drops and under agitation into 3.5 1 of ethyl acetate tor toluene). The precipitate is filtered and then washed 4 times with ethyl acetate and lastly vacuum dried for 24 hours at 30C. In this way 3.5 g of the compound named in the title are obtained.

Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, ~ohn Wiley and Sons Publication.

The degree of esterification is at least 99%.

SD 105 1 33823~

Example 43 - Preparation of the heDtadecYl ester of alginic acid 8.35 g (20 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from AscophYllum nodosum) are solubilized in 400 ml of DMS0 at 2SC.
8.0 g (25 m.Eq.) of heptadecyl bromide are added.

The solution is well agitated for 12 hours at 30C, and then slowly poured by regular drops and under agitation into 3.5 l of ethyl acetate (or toluene). The precipitate is filtered and then washed 4 times with ethyl acetate and lastly vacuum dried for 24 hours at 30C. In this way 4 g of the compound named in the title are obtained.

Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

- The degree of esterification is at least 99%.

SD 106 1 33823~

Example 441 - PreDaration of the octadecYl ester of alginic acid 8.3S g (20 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from Asco~h~llum nodosum) are solubilized in 400 ml of DMS0 at 25C.
8.37 g (25 m.Eq.) of octadecyl bromide are added.

The solution is well agitated for 12 hours at 30C, and then slowly poured by regular drops and under agitation into 3.5 1 of ethyl acetate (or toluene). The precipitate is filtered and then washed 4 times with ethyl acetate and lastly vacuum dried for 24 hours at 30C. In this way 3.5 g of the compound named in the title are obtained.

Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

- The degree of esterification is at least 99%.

SD 107 l 33B235 Example 45 - Preparation of the 3-Dhenylpropyl ester of al~inic acid 10 g (23.9 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from Laminaria hyper-borea) are solubilized in 400 ml of DMS0 at 25C.
5.18 g (26 m.Eq.) of 3-phenylpropyl bromide are added.

The solution is well agitated for 12 hours at 30C, and then slowly poured by regular drops and under agitation into 3.5 l of ethyl acetate (or toluene). The precipitate is filtered and then washed 4 times with ethyl acetate and lastly vacuum dried for 24 hours at 30C. In this way 4.0 g of the compound named in the title are obtained.

Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, 30hn Wiley and Sons Publication.

The degree of esterification is at least 99%.

Example 46 - PreParation of the 3,4,5-tr~methoxybenzyl estQr of al~inic acid 10 g (23.9 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from Laminaria hYper-borea) are solubilized in 400 ml of DMSO at 25C.
5.64 g (26 m.Eq.) of 3,4,5-trimethoxybenzyl chloride are added.

The solution is well agitated for 12 hours at 30C, and then slowly poured by regular drops and under agitation into 3.5 1 of ethyl acetate (or toluene). The precipitate is filtered and then washed 4 times with ethyl acetate and lastly vacuum dried for 24 hours at 30C. In this way 3.8 g of the compound named in the title are obtained.

Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of UQuantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

The degree of esterification is at least 9996.

Example 47 - Preparation of the cinn~myl ester of alqinic acid ._ 10 g (23.9 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from Laminaria hy~er-borea) are solubilized in 400 ml of DMSO at 25C.
5.15 g (26 m.Eq.) of cinnamyl bromide are added.

The solution is well agitated for 12 hours at 30C, and then slowly poured by regular drops and under agitation into 3.5 1 of ethyl acetate (or toluene). The precipitate is filtered and then washed 4 times with ethyl acetate and lastly vacuum dried for 24 hours at 30C. In this way 3.7 g of the compound named in the title are obtained.

Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of '~Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

The degree of esterification is at least 99%.

1 33823~

Example 48 - Preparation of the nonYl ester of al~inic acid 10 g (23.9 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from Laminaria hY~er-borea) are solubilized in 400 ml of DMS0 at 25C.
5.4 g (26 m.Eq.) of 1-bromononane are added.

The solution is well agitated for 12 hours at 30C, and then slowly poured by regular drops and under agitation into 3.5 l of ethyl acetate (or toluene). The precipitate is filtered and then washed 4 times with ethyl acetate and lastly vacuum dried for 24 hours at 30C. In this way 3.9 g of the compound named in the title are obtained.

Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of '!Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

The degree of esterification is at least 99%~

SD 111 1 3 3 8 2 3 :~

Example 49 - Preparation of the n-pentYlic ester of al~inic acid 10 g (23.9 m.Eq.) of the tetrabutylammonium salt of alginic acid (prepared from alginic acid obtained from Laminaria hYper-borea) are solubilized in 400 ml of DMS0 at 25C.
3.95 g (26 m.E~.) of n-pentyl bromide are added and 0.2 g of tetrabutylammonium iodide are added.

The solution is well agitated for 12 hours at 30C, and then slowly poured by regular drops and under agitation into 3.5 l of ethyl acetate (or toluene). The precipitate is filtered and then washed 4 times with ethyl acetate and lastly vacuum dried for 24 hours at 30C. In this way 3.8 g of the compound named in the title are obtained.

Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of "Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

The degree of esterification is at least 9g%.

1 3 3`~

Example 50i - PreParation of the isopentylic ester of alqinic acid 10 g (23.9 m.Eq.) of the tetra~utylammonium salt of alginic acid (prepared from alginic acid obtained from Laminaria hYPer-borea) are solubilized in 400 ml of DMS0 at 2SC.
3.95 g (26 m.Eq.) of isopentyl bromide are added and 0.2 g oftetrabutylammonium iodide are added.

The solution is well agitated for 12 hours at 30C, and then slowly poured by regular drops and under agitation into 3.5 1 of ethyl acetate (or toluene). The precipitate is filtered and then washed 4 times with ethyl acetate and lastly vacuum dried for 24 hours at 30C. In this way 3.8 g of the compound named in the title are obtained.

Quantitative determination of the ester groups is carried out by the saponification method described on pages 169-172 of ''Quantitative organic analysis via functional groups", 4th Edition, John Wiley and Sons Publication.

The degree of esterification is at least 99~.

' ' SD 113 3 33~2~5 Example 51 - PreParation of the (mixed) ethanolic and ~rednisolonic esters (C2t) of alginic acid - 80% of carboxylic ~roups esterified with ethanol - 20% of carboxylic ~roups esterified with prednisolone (C21).
4.18 g of the tetrabutylammonium salt of alginic acid (prepared from Macrocystis pyrifera) corresponding to 10 m.Eq. of a monomeric unit are solubilized in 210 ml of dimethylsulfoxide at 25C, 1.25g (8 m.Eq.) of ethyl iodide are added and the solution is kept for 24 hours at 30C.
0.85 g (2 m.Eq.) of 21-bromo-11,17-dihydroxypregnane-1,4 -diene-3,20-dione are added and the solution is kept for 24 hours at 30C.
A solution is then added containing 100 ml of water and 5 g of sodium chloride and the resulting mixture is slowly poured into 2,000 ml of acetone under constant agitation. A precipitate is formed which is filtered and washed three times with 100 ml of acetone/water 5:1 and three times with 100 ml of acetone and finally vacuum dried for eight hours at 30C.
1.7 g of the compound featured in the title are obtained.
Quantitative determination of prednisolone, after mild alkaline hydrolysis with hydroalcoholic solution of Na2C03 and extraction with chloroform, is carried out according to British Pharmacopeia.
Quantitative determination of the ethoxyls is carried out according to R. H. Cundiff and P.C. Markunas ~Anal. Chem. 33, 1028-1030 (1961)].
The degree of esterification is at least 99%.

; ~ . SD 114 1 338~35 Example 52 - Preparation of the (mixed) ethanolic and dex~-metha50nic esters (C21) of alginic acid - 80% of carboxylic qroups esterified with ethanol - 20% of carboxylic qrouPs e~terified with dexamethasone (C21~.
4.18 g of the tetrabutylammonium salt of alginic acid (prepared from Macrocystis pyrifera) corresponding to 10 m.E~. of a monomeric unit are solubilized in 210 ml of dimethylsulfoxide at 25C, 1.25g (8 m.Eq.) of ethyl iodide are added and the solution is kept for 24 hours at 30C.
0.91 g (2 m.Eq.) of 9-fluoro-21-bromo-11,17-dihydroxy-16-methylpregnane-1,4-diene-3,20-dione are added and the solution is kept for 24 hours at 30C.
A solution is then added containing 100 ml of water and 5 g of sodium chloride and the resulting mixture is slowly poured into 2,000 ml of acetone under constant agitation. A precipitate is formed which is filtered and washed three times with 100 ml of acetone/water 5:1 and three times with 100 ml of acetone and finally vacuum dried for eight hours at 30C.
1.6 g of the compound featured in the title are obtained.
Quantitative determination of dexamethasone, after mild alkaline hydrolysis with hydroalcoholic solution of Na2C03 and extraction with chloroform, is carried out according to British Pharmacopeia.
Quantitative determination of the ethoxyls is carried out according to R. H. Cundiff and P.C. Markunas ~Anal. Chem. 33, 1028-1030 (1961)].
The degree of esterification is at least 99%.

SD 115 l 3 3 8 2 3 5 ExamPle 53 - Preparation of the (mixed) ethanolic and cortisonic este~ tCzl) of alqinic acid - 80% of carboxYlic qroups esterified with ethanol - 20% of carboxylic qroups esterified with cortisone ( C21 ) .
4.18 g of the tetrabutylammonium salt of alginic acid (prepared from Macrocystis pyrifera) corresponding to 10 m.Eq. of a monomeric unit are solubilized in 210 ml of dimethylsulfoxide at 25C, 1.25g (8 m.Eq.) of ethyl iodide are added and the solution is kept for 24 hours at 30C.
0.85 g (2 m.Eq.) of 21-bromo-4-pregnane-17d-ol-3,11,30-trione are added and the solution is kept for 24 hours at 30C.
A solution is then added containing 100 ml of water and 5 g of sodium chloride and the resulting mixture is slowly poured into 2,000 ml of acetone under constant agitation. A precipitate is formed which is filtered and washed three times with 100 ml of acetone/water 5:1 and three times with 100 ml of acetone and finally vacuum dried for eight hours at 30C.
1.9 g of the compound featured in the title are obtained.
Quantitative determination of cortisone, after mild alkaline hydrolysis with hydroalcoholic solution of Na2C03 and extraction with chloroform, is carried out according to British Pharmacopeia.
Quantitative determination of the ethoxyls is carried out according to R. H. Cundiff and P.C. Markunas [Anal. Chem. 33, 1028-1030 (1961)].
The degree of esterification is at least 99%.

SD 116 1 3 ~ 8 ~ 3 5 _, Example 54 - PreParation of the (mixed) othanolic and hydro-corti~onic ester (C21) of al~nic acid - 80% of carboxylic ~L~V~
e~terified with ethanol - 20% of carboxylic ~roup~ esterified with hYdrocortisone (C21).
4.18 g of the tetrabutylammonium salt of alginic acid (prepared from Macrocystis pyrifera) corresponding to 10 m.Eq. of a monomeric unit are solubilized in 210 ml of dimethylsulfoxide at 25C, 1.25g (8 m.Eq.) of ethyl iodide are added and the solution is kept for 24 hours at 30C.
0.85 g (2 m.Eq.) of 21-bromo-4-pregnane-11~,17~-dial-3,20-dione are added and the solution is kept for 24 hours at 30C.
A solution is then added containing 100 ml of water and 5 g of sodium chloride and the resulting mixture is slowly poured into 2,000 ml of acetone under constant agitation. A precipitate is formed which is filtered and washed three times with 100 ml of acetone/water 5:1 and three times with 100 ml of acetone and finally vacuum dried for eight hours at 30C.
1.7 g of the compound featured in the title are obtained.
Quantitative determination of hydrocortisone, after mild alkaline hydrolysis with hydroalcoholic solution of Na2C03 and extraction with chloroform, is carried out according to British Pharmacopeia.
Quantitative determination of the ethoxyls is carried out according to R. H. Cundiff and P.C. Markunas tAnal. Chem. 33, 1028-1030 (1961)~.
The degree of esterification is at least 99%.

SD 117 1 33~35 ExamPle 55; - PreParation of the (mixed) ethanolic and desoxy-corticosteronic e~ter (Cz1) of al~inic acid - 80% of caroboxylic qrouPs esterified with ethanol - 20% of carboxylic ~rouPs e~teri-fied with desoxycorticosterone (C21).
4.18 g of the tetrabutylammonium salt of alginic acid (prepared from Laminaria hyperborea) corresponding to 10 m.Eq. of a monomeric unit are solubilized in 210 ml of dimethylsulfoxide at 25C, 1.25g (8 m.Eq.) of ethyl iodide are added and the solution is kept for 24 hours at 30C.
0.66 g (2 m.Eq.) of 21-bromo-4-pregnane-3,20-dione are added and the solution is kept for 24 hours at 30C.
A solution is then added containing 100 ml of water and 5 g of sodium chloride and the resulting mixture is slowly poured into 2,000 ml of acetone under constant agitation. A precipitate is formed which is filtered and washed three times with 100 ml of acetone/water 5:1 and three times with 100 ml of acetone and finally vacuum dried for eight hours at 30C.
1.9 g of the mixed ethanolic and desoxycorticosteronic ester compound featured in the title are obtained.
Quantitative determination of desoxycorticosteronic, after mild alkaline hydrolysis with hydroalcoholic solution of Na2CO3 and extraction with chloroform, is carried out according to British Pharmacopeia.
Quantitative determination of tne ethoxyls is carried out according to R. H. Cundiff and P.C. Markunas ~Anal. Chem. 33, 1028-1030 (1961)]. The degree of esterification is at least 99%.

Claims (88)

1. Sanitary or surgical articles comprising, as an essential component, at least one total, water-insoluble ester of alginic acid with an alcohol selected from the group consisting of aliphatic, araliphatic, cycloaliphatic, aliphatic-cycloaliphatic and heterocyclic alcohols, as well as possibly any incidental components which may have been used heretofore in sanitary or surgical articles.
2. The sanitary or surgical articles of claim 1 wherein, in said total, water-insoluble ester of alginic acid, said alcohol includes:
a) an aliphatic radical with a maximum of 34 carbon atoms;
b) an araliphatic radical with only one benzene ring, and in which the aliphatic chain therein has a maximum of 4 carbon atoms;
c) a cycloaliphatic radical which is monocyclic or polycyclic with a maximum of 34 carbon atoms;
d) an aliphatic-cycloaliphatic radical which is mono-cyclic or polycyclic with a maximum of 34 carbon atoms; or e) a heterocyclic radical with a maximum of 34 carbon atoms in which the hetero atoms are selected from the group consisting of oxygen, sulfur and nitrogen.
3. The sanitary or surgical articles of claim 2 wherein:
a) said aliphatic, cycloaliphatic, aliphatic-cyclo-aliphatic or heterocyclic radicals are substituted by one or two functional groups selected from the group consisting of amino, hydroxy, mercapto, aldehyde, keto, carboxyl, hydrocarbyl, dihydrocarbylamino, ether, ester, thioether, thioester, acetal, ketal, carbalkoxy and carbamidic groups, and carbamidic groups substituted by one or two alkyl groups, the hydrocarbyl radicals in these functional groups having a maximum of 6 carbon atoms; or b) said araliphatic radicals are substituted in the benzene residue with 1-3 substituents selected from the group consisting of methyl, hydroxy and halogen, or are substituted in the aliphatic portion with one or two functional groups selected from the group consisting of ethyl, diethyl, pyrrolidine and piperidine groups.
4. The sanitary or surgical articles of claim 3 wherein:
a) said hydrocarbyl radicals of said functional groups are C1-14 alkyl groups;
b) said amino or substituted carbamidic groups are C1-8 alkylene amine or C1-8 alkylene carbamidic groups; or c) said cycloaliphatic, aliphatic-cycloaliphatic or heterocyclic radicals are monocyclic with a maximum of 12 carbon atoms and the ring has between 5 and 7 carbon atoms.
5. Total, water-insoluble esters of alginic acid according to claim 2, wherein said aliphatic radical is derived from a compound selected from the group consisting of methyl alcohol, ethyl alcohol, propyl alcohol, isopropyl alcohol, n-butyl alcohol, isobutyl alcohol, tert-butyl alcohol, amyl alcohol, pentyl alcohol, hexyl alcohol, octyl alcohols glycerin, tartronic alcohol, lactic acids, gly-colic acid, malic acid, tartaric acid, citric acid, amino-ethanol, aminopropanol, n-aminobutanol or their dimethyl or diethyl derivatives in the amino radical, choline, pyrroli-dinylethanol, piperidinylethanol, piperazinylethanol, piperazinyl-n-propyl alcohol, piperazinyl-n-butyl alcohol, monothioethylene glycol, myricyl alcohol, citronellol, geraniol, nerol, nerolidol, linalool, farnesol and phytol.
6. The sanitary or surgical articles of claim 1 wherein said ester is the total, water-insoluble methyl ester of alginic acid.
7. The sanitary or surgical articles of claim 1 wherein said ester is the total, water-insoluble ethyl ester of alginic acid.
8. The sanitary or surgical articles of claim 1 wherein said ester is the total, water-insoluble isopropyl ester of alginic acid.
9. The sanitary or surgical articles of claim 1 wherein said ester is the total, water-insoluble tert-butyl ester of alginic acid.
10. The sanitary or surgical articles of claim 1 wherein said ester is the total, water-insoluble benzyl ester of alginic acid.
11. Sanitary or surgical articles according to claims 1 or 2, in the form of a film or thread, and in which any incidental component or components is, or are, one or ones, which has, or have, been used heretofore in surgical films or surgical threads.
12. Sanitary or surgical articles according to claims 3, 4 or 5 in the form of a film or thread, and in which any incidental component or components is, or are, one or ones, which has, or have, been used heretofore in surgical films or surgical threads.
13. Sanitary or surgical articles according to claims 6, 7 or 8 in the form of a film or thread, and in which any incidental component or components is, or are, one or ones, which has, or have, been used heretofore in surgical films or surgical threads.
14. Sanitary or surgical articles according to claims 9 or 10 in the form of a film or thread, and in which any incidental component or components is, or are, one or ones, which has, or have, been used heretofore in surgical films or surgical threads.
15. Sanitary or surgical articles according to claims 1 or 2 in the form of an artificial skin, and in which any incidental component or components is, or are, one or ones, which has, or have, been used heretofore in surgical films or surgical threads.
16. Sanitary or surgical articles according to claims 3, 4 or 5 in the form of an artificial skin, and in which any incidental component or components is, or are, one or ones, which has, or have, been used heretofore in surgical films or surgical threads.
17. Sanitary or surgical articles according to claims 6, 7 or 8 in the form of an artificial skin, and in which any incidental component or components is, or are, one or ones, which has, or have, been used heretofore in surgical films or surgical threads.
18. Sanitary or surgical articles according to claims 9 or 10 in the form of an artificial skin, and in which any incidental component or components is, or are, one or ones, which has, or have, been used heretofore in surgical films or surgical threads.
19. In a procedure for the preparation of sanitary or surgical articles in the form of films or threads the essential component of which comprises at least one total, water-insoluble ester of alginic acid with an alcohol selected from the group consisting of aliphatic, arali-phatic, cycloaliphatic, aliphatic-cycloaliphatic and heterocyclic alcohols, the essential steps of said proce-dure comprising: dissolving said total, water-insoluble alginic ester in a first organic solvent; making said solution into sheet form or thread form, respectively; then eliminating said first organic solvent by treatment with a second suitable organic or with an aqueous solvent which is soluble in said first solvent; and then removing said second organic or aqueous solvent.
20. The procedure of claim 19 wherein, in said total, water-insoluble ester of alginic acid, said alcohol includes:
a) an aliphatic radical with a maximum of 34 carbon atoms;

b) an araliphatic radical with only one benzene ring, and in which the aliphatic chain therein has a maximum of 4 carbon atoms;
c) a cycloaliphatic radical which is monocyclic or polycyclic with a maximum of 34 carbon atoms;
d) an aliphatic-cycloaliphatic radical which is monocyclic or polycyclic with a maximum of 34 carbon atoms;
or e) a heterocyclic radical with a maximum of 34 carbon atoms in which the hetero atoms are selected from the group consisting of oxygen, sulfur and nitrogen.
21. The procedure of claim 20 wherein:
a) said aliphatic, cycloaliphatic, aliphatic-cyclo-aliphatic or heterocyclic radicals are substituted by one or two functional groups selected from the group consisting of amino, hydroxy, mercapto, aldehyde, keto, carboxyl, hydrocarbyl, dihydrocarbylamino, ether, ester, thioether, thioester, acetal, ketal, carbalkoxy and carbamidic groups and carbamidic groups substituted by one or two alkyl groups, the hydrocarbyl radicals in these functional groups having a maximum of 6 carbon atoms; or b) said araliphatic radicals are substituted in the benzene residue with 1-3 substituents selected from the group consisting of methyl, hydroxy and halogen, or are substituted in the aliphatic portion with one or two func-tional groups selected from the group consisting of ethyl, diethyl, pyrrolidine and piperidine groups.
22. The procedure of claim 21 wherein:

a) said hydrocarbyl radicals of said functional groups are C1-14 alkyl groups;
b) said amino or substituted carbamidic groups are C1-8 alkylene amine or C1-8 alkylene carbamidic groups; or c) said cycloaliphatic, aliphatic-cycloaliphatic or heterocyclic radicals are monocyclic with a maximum of 12 carbon atoms and the ring has between 5 and 7 carbon atoms.
23. The procedure of claim 20 wherein said aliphatic radical is derived from a compound selected from the group consisting of methyl alcohol, ethyl alcohol, propyl alcohol, isopropyl alcohol, n-butyl alcohol, isobutyl alcohol, tert-butyl alcohol, amyl alcohol, pentyl alcohol, hexyl alcohol, octyl alcohols glycerin, tartronic alcohol, lactic acids, glycolic acid, malic acid, tartaric acid, citric acid, aminoethanol, aminopropanol, n-aminobutanol or their dimethyl or diethyl derivatives in the amino moiety, choline, pyrrolidinylethanol, piperidinylethanol, piper-azinylethanol,piperazinyl-n-propyl alcohol, piperazinyl-n-butyl alcohol, monothioethylene glycol, myricyl alcohol, citronellol, geraniol, nerol, nerolidol, linalool, farnesol and phytol.
24. The procedure of claim 19 wherein said ester is the total, water-insoluble methyl ester of alginic acid.
25. The procedure of claim 19 wherein said ester is the total, water-insoluble ethyl ester of alginic acid.
26. The procedure of claim 19 wherein said ester is the total, water-insoluble isopropyl ester of alginic acid.
27. The procedure of claim 19 wherein said ester is the total, water-insoluble tert-butyl ester of alginic acid.

126
28. Sanitary or surgical articles the essential component of which comprises at least one total, water-insoluble ester of alginic acid with an alcohol selected from the group consisting of cyclohexyl alcohol, sec-butyl alcohol, cyclobutyl alcohol, decyl alcohol, dodecyl alcohol, 2-phenylethyl alcohol, heptyl alcohol, hexyl alcohol, propyl alcohol, n-octyl alcohol, 2,6-dichloro-benzyl alcohol, 4-tert-butylbenzyl alcohol, heptadecyl alcohol, octadecyl alcohol, 3-phenylpropyl alcohol, 3,4,5-trimethoxybenzyl alcohol, cinnamyl alcohol, nonyl alcohol, n-pentylic alcohol, isopentylic alcohol, a mixture of ethyl and prednisolonyl alcohols, a mixture of ethyl and dexa-methasonyl alcohols, a mixture of ethyl and cortisonyl alcohols, a mixture of ethyl and hydrocortisonyl alcohols, and a mixture of ethyl and desoxycorticosteronyl alcohols, as well as possibly any incidental ingredients which may have been used heretofore in sanitary or surgical articles.
29. The sanitary or surgical articles of claim 28 wherein said ester is derived from an alcohol selected from the group consisting of cyclohexyl alcohol, sec-butyl alcohol, cyclobutyl alcohol, decyl alcohol, dodecyl alcohol, 2-phenylethyl alcohol, heptyl alcohol, hexyl alcohol, propyl alcohol, n-octyl alcohol, 2,6-dichlorobenzyl, 4-tert-butylbenzyl alcohol, heptadecyl alcohol, octadecyl alcohol, 3-phenylpropyl alcohol, 3,4,5-trimethoxybenzyl alcohol, cinnamyl alcohol, nonyl alcohol, n-pentylic alcohol, and isopentylic alcohol.
30. The sanitary or surgical articles of claim 28 wherein said ester is derived from alcohols selected from the group consisting of a mixture of ethyl and predniso-lonyl alcohols, a mixture of ethyl and dexamethasonyl alcohols, a mixture of ethyl and cortisonyl alcohols, a mixture of ethyl and hydrocortisonyl alcohols, and a mixture of ethyl and desoxycorticosteronyl alcohols.
31. The sanitary or surgical articles of claim 28 wherein said ester is selected from the group consisting of the (mixed) ethanolic and prednisolonic esters (C21) of alginic acid - 80% of carboxylic groups esterified with ethanol -20% of carboxylic groups esterified with predniso-lone (C21); the (mixed) ethanolic and dexamethasonic esters (C21) of alginic acid - 80% of carboxylic groups esterified with ethanol -20% of carboxylic groups esterified with dexamethasone (C21); the (mixed) ethanolic and cortisonic esters (C21) of alginic acid - 80% of carboxylic groups esterified with ethanol - 20% of carboxylic groups esteri-fied with cortisone (C21); the (mixed) ethanolic and hydro-cortisonic esters (C21) of alginic acid - 80% of carboxylic groups esterified with ethanol - 20% of carboxylic groups esterified with hydrocortisone (C21); and the (mixed) ethanolic and desoxycorticosteronic esters (C21) of alginic acid - 80% of carboxylic groups esterified with ethanol -20% of carboxylic groups esterified with desoxycorticos-terone (C21).
32. The sanitary or surgical articles of claim 29 wherein said ester is the total, water-insoluble cyclohexyl ester of alginic acid.
33. The sanitary or surgical articles of claim 29 wherein said ester is the total, water-insoluble sec-butyl ester of alginic acid.
34. The sanitary or surgical articles of claim 29 wherein said ester is the total, water-insoluble cyclobutyl ester of alginic acid.
35. The sanitary or surgical articles of claim 29 wherein said ester is the total, water-insoluble decyl ester of alginic acid.
36. The sanitary or surgical articles of claim 29 wherein said ester is the total, water-insoluble dodecyl ester of alginic acid.
37. The sanitary or surgical articles of claim 29 wherein said ester is the total, water-insoluble 2-phenyl-ethyl ester of alginic acid.
38. The sanitary or surgical articles of claim 29 wherein said ester is the total, water-insoluble heptyl ester of alginic acid.
39. The sanitary or surgical articles of claim 29 wherein said ester is the total, water-insoluble hexyl ester of alginic acid.
40. The sanitary or surgical articles of claim 29 wherein said ester is the total, water-insoluble propyl ester of alginic acid.
41. The sanitary or surgical articles of claim 29 wherein said ester is the total, water-insoluble n-octyl ester of alginic acid.
42. The sanitary or surgical articles of claim 29 wherein said ester is the total, water-insoluble 2,6-dichlorobenzyl ester of alginic acid.
43. The sanitary or surgical articles of claim 29 wherein said ester is the total, water-insoluble 4-tert-butylbenzyl ester of alginic acid.
44. The sanitary or surgical articles of claim 29 wherein said ester is the total, water-insoluble heptadecyl ester of alginic acid.
45. The sanitary or surgical articles of claim 29 wherein said ester is the total, water-insoluble octadecyl ester of alginic acid.
46. The sanitary or surgical articles of claim 29 wherein said ester is the total, water-insoluble 3-phenyl-propyl ester of alginic acid.
47. The sanitary or surgical articles of claim 29 wherein said ester is the total, water-insoluble 3,4,5-trimethoxybenzyl ester of alginic acid.
48. The sanitary or surgical articles of claim 29 wherein said ester is the total, water-insoluble cinnamyl ester of alginic acid.
49. The sanitary or surgical articles of claim 29 wherein said ester is the total, water-insoluble nonyl ester of alginic acid.
50. The sanitary or surgical articles of claim 29 wherein said ester is the total, water-insoluble n-pentylic ester of alginic acid.
51. The sanitary or surgical articles of claim 29 wherein said ester is the total, water-insoluble isopen-tylic ester of alginic acid.
52. The sanitary or surgical articles of claim 31 wherein said ester is the total, water-insoluble mixed ethanolic and prednisolonic esters (C21) of alginic acid, in which 80% of carboxylic groups are esterified with ethanol, and in which 20% of carboxylic groups are esterified with prednisolone (C21).
53. The sanitary or surgical articles of claim 31 wherein said ester is the total, water-insoluble mixed ethanolic and dexamethasonic esters (C21) of alginic acid, in which 80% of carboxylic groups are esterified with ethanol, and in which 20% of carboxylic groups are esteri-fied with dexamethasone (C21).
54. The sanitary or surgical articles of claim 30 wherein said ester is the total, water-insoluble mixed ethanolic and cortisonic esters (C21) of alginic acid, in which 80% of carboxylic groups are esterified with ethanol, and in which 20% of carboxylic groups are esterified with cortisone (C21).
55. The sanitary or surgical articles of claim 28 wherein said ester is the total, water-insoluble mixed ethanolic and hydrocortisonic esters (C21) of alginic acid, in which 80% of carboxylic groups are esterified with ethanol, and in which 20% of carboxylic groups are esteri-fied with hydrocortisone (C21).
56. The sanitary or surgical articles of claim 28 wherein said ester is the total, water-insoluble mixed ethanolic and desoxycorticosteronic esters (C21) of alginic acid, in which 80% of carboxylic groups are esterified with ethanol, and in which 20% of carboxylic groups are esteri-fied with desoxycorticosterone (C21).
57. Sanitary or surgical articles according to claims 29, 30 or 31, in the form of a film or thread, and in which any incidental component or components is, or are, one or ones, which has, or have, been used heretofore in surgical films or surgical threads.
58. Sanitary or surgical articles according to claims 32, 33 or 34, in the form of a film or thread, and in which any incidental component or components is, or are, one or ones, which has, or have, been used heretofore in surgical films or surgical threads.
59. Sanitary or surgical articles according to claims 35, 36 or 37 in the form of a film or thread, and in which any incidental component or components is, or are, one or ones, which has, or have, been used heretofore in surgical films or surgical threads.
60. Sanitary or surgical articles according to claims 38, 39 or 40 in the form of a film or thread, and in which any incidental component or components is, or are, one or ones, which has, or have, been used heretofore in surgical films or surgical threads.
61. Sanitary or surgical articles according to claims 41, 42 or 43 in the form of a film or thread, and in which any incidental component or components is, or are, one or ones, which has, or have, been used heretofore in surgical films or surgical threads.
62. Sanitary or surgical articles according to claims 44, 45 or 46 in the form of a film or thread, and in which any incidental component or components is, or are, one or ones, which has, or have, been used heretofore in surgical films or surgical threads.
63. Sanitary or surgical articles according to claims 47, 48 or 49 in the form of a film or thread, and in which any incidental component or components is, or are, one or ones, which has, or have, been used heretofore in surgical films or surgical threads.
64. Sanitary or surgical articles according to claims 50, 51 or 52 in the form of a film or thread, and in which any incidental component or components is, or are, one or ones, which has, or have, been used heretofore in surgical films or surgical threads.
65. Sanitary or surgical articles according to claims 53 or 54 in the form of a film or thread, and in which any incidental component or components is, or are, one or ones, which has, or have, been used heretofore in surgical films or surgical threads.
66. Sanitary or surgical articles according to claims 55 or 56 in the form of a film or thread, and in which any incidental component or components is, or are, one or ones, which has, or have, been used heretofore in surgical films or surgical threads.
67. Sanitary or surgical articles according to claims 29, 30 or 31 in the form of an artificial skin, and in which any incidental component or components is, or are, one or ones, which has, or have, been used heretofore in surgical films or surgical threads.
68. Sanitary or surgical articles according to claims 32, 33 or 34 in the form of an artificial skin, and in which any incidental component or components is, or are, one or ones, which has, or have, been used heretofore in surgical films or surgical threads.
69. Sanitary or surgical articles according to claims 35, 36 or 37 in the form of an artificial skin, and in which any incidental component or components is, or are, one or ones, which has, or have, been used heretofore in surgical films or surgical threads.
70. Sanitary or surgical articles according to claims 38, 39 or 40 in the form of an artificial skin, and in which any incidental component or components is, or are, one or ones, which has, or have, been used heretofore in surgical films or surgical threads.
71. Sanitary or surgical articles according to claims 41, 42 or 43 in the form of an artificial skin, and in which any incidental component or components is, or are, one or ones, which has, or have, been used heretofore in surgical films or surgical threads.
72. Sanitary or surgical articles according to claims 44, 45 or 46 in the form of an artificial skin, and in which any incidental component or components is, or are, one or ones, which has, or have, been used heretofore in surgical films or surgical threads.
73. Sanitary or surgical articles according to claims 47, 48 or 49 in the form of an artificial skin, and in which any incidental component or components is, or are, one or ones, which has, or have, been used heretofore in surgical films or surgical threads.
74. Sanitary or surgical articles according to claims 50, 51 or 52 in the form of an artificial skin, and in which any incidental component or components is, or are, one or ones, which has, or have, been used heretofore in surgical films or surgical threads.
75. Sanitary or surgical articles according to claims 53 or 54 in the form of an artificial skin, and in which any incidental component or components is, or are, one or ones, which has, or have, been used heretofore in surgical films or surgical threads.
76. Sanitary or surgical articles according to claims 55 or 56 in the form of an artificial skin, and in which any incidental component or components is, or are, one or ones, which has, or have, been used heretofore in surgical films or surgical threads.
77. In a procedure for the preparation of sanitary or surgical articles in the form of films or threads the essential component of which comprises at least one total water-insoluble ester of alginic acid with an alcohol selected from the group consisting of cyclohexyl alcohol, sec-butyl alcohol, cyclobutyl alcohol, decyl alcohol, dodecyl alcohol, 2-phenylethyl alcohol, heptyl alcohol, hexyl alcohol, propyl alcohol, n-octyl alcohol, 2,6-di-chlorobenzyl alcohol, 4-tert-butylbenzyl alcohol, heptadecyl alcohol, octadecyl alcohol, 3-phenylpropyl alcohol, 3,4,5-trimethoxybenzyl alcohol, cinnamyl alcohol, nonyl alcohol, n-pentylic alcohol, isopentylic alcohol, a mixture of ethyl and prednisolonyl alcohols, a mixture of ethyl and dexamethasonyl alcohols, a mixture of ethyl and cortisonyl alcohols, a mixture of ethyl and hydrocortisonyl alcohols, and a mixture of ethyl and desoxycorticosteronyl alcohols, the essential steps of said procedure comprising:
dissolving said total, water-insoluble alginic ester in a first organic solvent; making said solution into sheet or thread form respectively; then eliminating said first organic solvent by treatment with a second suitable organic or with an aqueous solvent which is soluble in said first solvent; and then removing said second organic or aqueous solvent.
78. The procedure of claim 77 wherein, in said total, water-insoluble ester of alginic acid, said alcohol is selected from the group consisting of cyclohexyl alcohol, sec-butyl alcohol, cyclobutyl alcohol, decyl alcohol, dodecyl alcohol, 2-phenylethyl alcohol, heptyl alcohol, hexyl alcohol, propyl alcohol, n-octyl alcohol, 2,6-dichlorobenzyl alcohol, 4-tert-butylbenzyl alcohol, heptadecyl alcohol, octadecyl alcohol, 3-phenylpropyl alcohol, 3,4,5-trimethoxybenzyl alcohol, cinnamyl alcohol, nonyl alcohol, n-pentylic alcohol, and isopentylic alcohol.
79. The procedure of claim 77 wherein, in said total, water-insoluble ester of alginic acid, said alcohols are selected from the group consisting of a mixture of ethyl and prednisolonyl alcohols, a mixture of ethyl and dexa-methasonyl alcohols, a mixture of ethyl and cortisonyl alcohols, a mixture of ethyl and hydrocortisonyl alcohols, and a mixture of ethyl and desoxycorticosteronyl alcohols.
80. The procedure of claim 77 wherein, in said total, water-insoluble ester of alginic acid, is selected from the group consisting of the (mixed) ethanolic and prednisolonic esters (C21) of alginic acid - 80% of carboxylic groups esterified with ethanol -20% of carboxylic groups esteri-fied with prednisolone (C21); the (mixed) ethanolic and dexamethasonic esters (C21) of alginic acid - 80% of carboxylic groups esterified with ethanol - 20% of carboxy-lic groups esterified with dexamethasone (C21); the (mixed) ethanolic and cortisonic esters (C21) of alginic acid - 80%
of carboxylic groups esterified with ethanol - 20% of carboxylic groups esterified with cortisone (C21); the (mixed) ethanolic and hydrocortisonic esters (C21) of alginic acid - 80% of carboxylic groups esterified with ethanol - 20% of carboxylic groups esterified with hydro-cortisone (C21); and the (mixed) ethanolic and desoxycorti-costeronic esters (C21) of alginic acid - 80% of carboxylic groups esterified with ethanol - 20% of carboxylic groups esterified with desoxycorticosterone (C21).
81. A method for using threads, the essential component of which comprises at least one total, water-insoluble esters of alginic acid with an alcohol, selected from the groups consisting of cyclohexyl alcohol, sec-butyl alcohol, cyclobutyl alcohol, decyl alcohol, dodecyl alcohol, 2-phenylethyl alcohol, heptyl alcohol, hexyl alcohol, propyl alcohol, n-octyl alcohol, 2,6-dichloro-benzyl alcohol, 4-tert-butylbenzyl alcohol, heptadecyl alcohol, octadecyl alcohol, 3-phenylpropyl alcohol, 3,4,5-trimethoxybenzyl alcohol, cinnamyl alcohol, nonyl alcohol, n-pentylic alcohol, isopentylic alcohol, a mixture of ethyl and prednisolonyl alcohols, a mixture of ethyl and dexa-méthasonyl alcohols, a mixture of ethyl and cortisonyl alcohols, a mixture of ethyl and hydrocortisonyl alcohols, and a mixture of ethyl and desoxycorticosteronyl alcohols, which procedure comprises: dissolving said total, water-insoluble alginic ester in a first organic solvent; making said solution into thread form; then eliminating said first organic solvent by treatment with a second suitable organic or with an aqueous solvent which is soluble in said first solvent; then removing said second organic or aqueous solvent; and then using said threads as well as possibly any incidental ingredients which may have been used heretofore as suture threads in surgical articles in surgical operations.
82. The method of claim 81 wherein, in said total, water-insoluble ester of alginic acid, said alcohol is selected from the group consisting of cyclohexyl alcohol, sec-butyl alcohol, cyclobutyl alcohol, decyl alcohol, dodecyl alcohol, 2-phenylethyl alcohol, heptyl alcohol, hexyl alcohol, propyl alcohol, n-octyl alcohol, 2,6-dichlorobenzyl alcohol, 4-tert-butylbenzyl alcohol, heptadecyl alcohol, octadecyl alcohol, 3-phenylpropyl alcohol, 3,4,5-trimethoxybenzyl alcohol, cinnamyl alcohol, nonyl alcohol, n-pentylic alcohol, and isopentylic alcohol.
83. The method of claim 81 wherein, in said total, water-insoluble ester of alginic acid, said alcohol is selected from the group consisting of a mixture of ethyl and prednisolonyl alcohols, a mixture of ethyl and dexa-méthasonyl alcohols, a mixture of ethyl and cortisonyl alcohols, a mixture of ethyl and hydrocortisonyl alcohols, and a mixture of ethyl and desoxycorticosteronyl alcohols.
84. The method of claim 81 wherein, said total, water-insoluble ester of alginic acid, is selected from the group consisting of the (mixed) ethanolic and prednisolonic esters (C21) of alginic acid - 80% of carboxylic groups esterified with ethanol - 20% of carboxylic groups esteri-fied with prednisolone (C21); the (mixed) ethanolic and dexamethasonic esters (C21) of alginic acid - 80% of carboxylic groups esterified with ethanol - 20% of carboxylic groups esterified with dexamethasone (C21); the (mixed) ethanolic and cortisonic esters (C21) of alginic acid - 80% of carboxylic groups esterified with ethanol -20% of carboxylic groups esterified with cortisone (C21);
the (mixed) ethanolic and hydrocortisonic esters (C21) of alginic acid - 80% of carboxylic groups esterified with ethanol -20% of carboxylic groups esterified with hydro-cortisone (C21); and the (mixed) ethanolic and desoxycorti-costeronic esters (C21) of alginic acid - 80% of carboxylic groups esterified with ethanol - 20% of carboxylic groups esterified with desoxycorticosterone (C21).
85. A method for using films, the essential component of which comprises at least one total, water-insoluble ester of alginic acid with an alcohol, selected from the group consisting of cyclohexyl alcohol, sec-butyl alcohol, cyclobutyl alcohol, decyl alcohol, dodecyl alcohol, 2-phenylethyl alcohol, heptyl alcohol, hexyl alcohol, propyl alcohol, n-octyl alcohol, 2,6-dichlorobenzyl alcohol, 4-tert-butylbenzyl alcohol, heptadecyl alcohol, octadecyl alcohol, 3-phenylpropyl alcohol, 3,4,5-trimethoxybenzyl alcohol, cinnamyl alcohol, nonyl alcohol, n-pentylic alcohol, isopentylic alcohol, a mixture of ethyl and prednisolonyl alcohols, a mixture of ethyl and dexa-methasonyl alcohols, a mixture of ethyl and cortisonyl alcohols, a mixture of ethyl and hydrocortisonyl alcohols, and a mixture of ethyl and desoxycorticosteronyl alcohols, which procedure comprises: dissolving said total, water-insoluble alginic ester in a first organic solvent; making said solution into sheet form; then eliminating said first organic solvent by treatment with a second suitable organic solvent or with an aqueous solvent which is soluble in said first solvent; then removing said second organic or aqueous solvent; and then using said film, as well as possibly any incidental ingredients which may have been used heretofore in surgical articles, as artificial skin.
86. The method of claim 85 wherein, in said total, water-insoluble ester of alginic acid, said alcohol is selected from the group consisting of cyclohexyl alcohol, sec-butyl alcohol, cyclobutyl alcohol, decyl alcohol, dodecyl alcohol, 2-phenylethyl alcohol, heptyl alcohol, hexyl alcohol, propyl alcohol, n-octyl alcohol, 2,6-dichlorobenzyl alcohol, 4-tert-butylbenzyl alcohol, heptadecyl alcohol, octadecyl alcohol, 3-phenylpropyl alcohol, 3,4,5-trimethoxybenzyl alcohol, cinnamyl alcohol, nonyl alcohol, n-pentylic alcohol, and isopentylic alcohol.
87. The method of claim 85 wherein, in said total, water-insoluble ester of alginic acid, said alcohol is selected from the group consisting of a mixture of ethyl and prednisolonyl alcohols, a mixture of ethyl and dexa-methasonyl alcohols, a mixture of ethyl and cortisonyl alcohols, a mixture of ethyl and hydrocortisonyl alcohols, and a mixture of ethyl and desoxycorticosteronyl alcohols.
88. The method of claim 85 wherein said total, water-insoluble ester of alginic acid is selected from the group consisting of the (mixed) ethanolic and prednisolonic esters (C21) of alginic acid - 80% of carboxylic groups esterified with ethanol - 20% of carboxylic groups esterified with prednisolone (C21); the (mixed) ethanolic and dexamethasonic esters (C21) of alginic acid - 80% of carboxylic groups esterified with ethanol - 20% of carboxylic groups esterified with dexamethasone (C21); the (mixed) ethanolic and cortisonic esters (C21) of alginic acid - 80% of carboxylic groups esterified with ethanol -20% of carboxylic groups esterified with cortisone (C21);
the (mixed) ethanolic and hydrocortisonic esters (C21) of alginic acid - 80% of carboxylic groups esterified with ethanol - 20% of carboxylic groups esterified with hydro-cortisone (C21); and the (mixed) ethanolic and desoxycorti-costeronic esters (C21) of alginic acid - 80% of carboxylic groups esterified with ethanol - 20% of carboxylic groups esterified with desoxycorticosterone (C21).
CA000540467A 1986-06-30 1987-06-24 Esters of alginic acid Expired - Fee Related CA1338235C (en)

Priority Applications (1)

Application Number Priority Date Filing Date Title
CA000616909A CA1338236C (en) 1986-06-30 1994-08-22 Esters of alginic acid

Applications Claiming Priority (2)

Application Number Priority Date Filing Date Title
IT48201/86A IT1203814B (en) 1986-06-30 1986-06-30 ESTERS OF ALGINIC ACID
IT48201A/86 1986-06-30

Related Child Applications (1)

Application Number Title Priority Date Filing Date
CA000616909A Division CA1338236C (en) 1986-06-30 1994-08-22 Esters of alginic acid

Publications (1)

Publication Number Publication Date
CA1338235C true CA1338235C (en) 1996-04-09

Family

ID=11265177

Family Applications (1)

Application Number Title Priority Date Filing Date
CA000540467A Expired - Fee Related CA1338235C (en) 1986-06-30 1987-06-24 Esters of alginic acid

Country Status (24)

Country Link
US (1) US5336668A (en)
EP (2) EP0609968A3 (en)
JP (2) JP2569054B2 (en)
CN (1) CN1026001C (en)
AR (1) AR242959A1 (en)
AT (1) ATE113610T1 (en)
AU (2) AU602901B2 (en)
CA (1) CA1338235C (en)
DE (1) DE3750710T2 (en)
DK (1) DK333687A (en)
EG (1) EG18197A (en)
FI (1) FI872878A (en)
HU (1) HU202559B (en)
IL (1) IL82943A (en)
IN (1) IN166549B (en)
IT (1) IT1203814B (en)
MX (1) MX7108A (en)
NO (1) NO175059B (en)
NZ (1) NZ220807A (en)
PH (1) PH25729A (en)
PL (1) PL157922B1 (en)
PT (1) PT85200B (en)
YU (2) YU46960B (en)
ZA (1) ZA874520B (en)

Families Citing this family (57)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US5264422A (en) * 1986-06-30 1993-11-23 Fidia S.P.A. Esters of alginic acid with steroidal alcohols
DK110188D0 (en) * 1988-03-02 1988-03-02 Claus Selch Larsen HIGH MOLECULAR WEIGHT PRODRUG DERIVATIVES OF ANTI-FLAMMATORY DRUGS
IT1219942B (en) * 1988-05-13 1990-05-24 Fidia Farmaceutici POLYSACCHARIDIC ESTERS
JP2627344B2 (en) * 1990-01-23 1997-07-02 工業技術院長 Water-soluble algin fiber and method for producing the same
CA2061016A1 (en) * 1991-02-11 1992-08-12 Francesco Della Valle Gellan esters
IT1247472B (en) * 1991-05-31 1994-12-17 Fidia Spa PROCESS FOR THE PREPARATION OF MICROSPHERES CONTAINING BIOLOGICALLY ACTIVE COMPONENTS.
IT1263755B (en) * 1991-09-16 1996-08-29 Fidia Spa USE OF CHINA ESTERS WITH ACID POLYSACCHARIDES AS ANTI-ULCER AND GASTROPROTECTIVE AGENTS
EP0610441A4 (en) * 1991-10-29 1996-01-10 Clover Cons Ltd Crosslinkable polysaccharides, polycations and lipids useful for encapsulation and drug release.
IT1254704B (en) * 1991-12-18 1995-10-09 Mini Ricerca Scient Tecnolog NON-WOVEN FABRIC ESSENTIALLY CONSTITUTED FROM DERIVATIVES OF HYALURONIC ACID
US5824335A (en) * 1991-12-18 1998-10-20 Dorigatti; Franco Non-woven fabric material comprising auto-crosslinked hyaluronic acid derivatives
IT1254170B (en) * 1991-12-18 1995-09-11 Mini Ricerca Scient Tecnolog COMPOSITE MEMBRANES FOR GUIDED REGENERATION OF FABRICS
FR2699545B1 (en) * 1992-12-18 1995-01-27 Oreal Gelling agent resulting from the combination of a chitosan and an alkyl or hydroxyalkyl alginate and its use in the preparation of cosmetic and pharmaceutical compositions.
IT1263394B (en) * 1993-07-30 1996-08-05 Fidia Advanced Biopolymers Srl PHARMACEUTICAL COMPOSITIONS FOR TOPICAL USE BASED ON HYALURONIC ACID AND ITS DERIVATIVES
IT1268955B1 (en) * 1994-03-11 1997-03-18 Fidia Advanced Biopolymers Srl ACTIVE ESTERS OF CARBOXYL POLYSACCHARIDES
IL114193A (en) * 1994-06-20 2000-02-29 Teva Pharma Ophthalmic pharmaceutical compositions based on sodium alginate
CA2212519C (en) * 1995-02-07 2005-08-23 Fidia Advanced Biopolymers, S.R.L. Process for the coating of objects with hyaluronic acid, derivatives thereof, and semisynthetic polymers
IT1281886B1 (en) * 1995-05-22 1998-03-03 Fidia Advanced Biopolymers Srl PROCESS FOR THE PREPARATION OF HYDROGELS OBTAINED FROM CHEMICAL DERIVATIVES OF HYALURONIC ACID BY MEANS OF ULTRAVIOLET IRRADIATION AND THEIR
FR2764505B1 (en) * 1997-06-13 1999-10-15 Alain Dogliani NOVEL COSMETIC COMPOSITIONS BASED ON ALKALINE ALGINATE LYOPHILISATES AND NEW PENETRATION VECTORS
IT1294797B1 (en) 1997-07-28 1999-04-15 Fidia Advanced Biopolymers Srl USE OF HYALURONIC ACID DERIVATIVES IN THE PREPARATION OF BIOMATERIALS WITH PHYSICAL AND BUFFERING HEMOSTATIC ACTIVITIES
FR2778081B1 (en) * 1998-04-29 2000-08-25 Fabrice Thevenet REINFORCEMENT IMPLANTS FOR TISSUE SUTURES
FR2781677B1 (en) * 1998-07-31 2000-10-20 Brothier Lab WOUND TREATMENT DEVICE AND METHOD FOR MANUFACTURING THIS DEVICE
WO2000021572A2 (en) 1998-10-09 2000-04-20 The University Of Michigan Hydrogels and water soluble polymeric carriers for drug delivery
DE10112825A1 (en) 2001-03-16 2002-10-02 Fresenius Kabi De Gmbh HESylation of active ingredients in aqueous solution
JP3814224B2 (en) * 2001-04-25 2006-08-23 エーザイ株式会社 Composition for external use
DE10209821A1 (en) 2002-03-06 2003-09-25 Biotechnologie Ges Mittelhesse Coupling of proteins to a modified polysaccharide
DE10209822A1 (en) 2002-03-06 2003-09-25 Biotechnologie Ges Mittelhesse Coupling of low molecular weight substances to a modified polysaccharide
PL217085B1 (en) 2002-09-11 2014-06-30 Fresenius Kabi Gmbh Hasylated polypeptides, especially hasylated erythropoietin
AU2003273413A1 (en) 2002-10-08 2004-05-04 Fresenius Kabi Deutschland Gmbh Pharmaceutically active oligosaccharide conjugates
FR2850281A1 (en) * 2003-01-27 2004-07-30 Brothier Lab Production of a suture-reinforcing device comprises coating a guluronic-type calcium alginate textile material with a solution of propylene glycol alginate with a high degree of esterification
US7008476B2 (en) 2003-06-11 2006-03-07 Az Electronic Materials Usa Corp. Modified alginic acid of alginic acid derivatives and thermosetting anti-reflective compositions thereof
WO2005014655A2 (en) 2003-08-08 2005-02-17 Fresenius Kabi Deutschland Gmbh Conjugates of hydroxyalkyl starch and a protein
GB2404920A (en) * 2003-08-12 2005-02-16 Johnson & Johnson Medical Ltd Antimicrobial polymer
AU2004275594A1 (en) * 2003-09-30 2005-04-07 Solubest Ltd. Water soluble nanoparticles inclusion complexes
DE202005021885U1 (en) 2004-03-11 2011-03-03 Fresenius Kabi Deutschland Gmbh Hydroxyalkyl starch-protein conjugates prepared by reductive amination
PE20060468A1 (en) * 2004-04-26 2006-07-06 Cp Kelco Aps DERMOPROTECTIVE COMPOSITION TO CONTROL SKIN ALKALINITY, INCLUDING CARBOXYLIC ACID POLYSACCHARIDS
DE102004025495A1 (en) 2004-05-21 2005-12-15 Dr. Suwelack Skin & Health Care Ag Process for the production of alginate-containing porous moldings
GB0513552D0 (en) 2005-07-01 2005-08-10 Bristol Myers Squibb Co Bandage
DE102005049833A1 (en) * 2005-10-14 2007-04-19 Beiersdorf Ag New alginate, in which carboxylic acid functional groups are partially esterified or etherified with an alkyl and/or aryl residue, useful for reducing the stickiness of cosmetic preparation
EP2070950A1 (en) 2007-12-14 2009-06-17 Fresenius Kabi Deutschland GmbH Hydroxyalkyl starch derivatives and process for their preparation
FR2936800B1 (en) * 2008-10-06 2010-12-31 Adocia POLYSACCHARIDE COMPRISING FUNCTIONAL CARBOXYL GROUPS SUBSTITUTED WITH A HYDROPHOBIC ALCOHOL DERIVATIVE
US8426382B2 (en) 2008-10-06 2013-04-23 Adocia Polysaccharides comprising carboxyl functional groups substituted by a hydrophobic alcohol derivative
JP2010106068A (en) * 2008-10-28 2010-05-13 Mie Prefecture New chemical modification method for polysaccharide
WO2010069519A1 (en) * 2008-12-18 2010-06-24 Merz Pharma Gmbh & Co. Kgaa Topical compositions comprising at least one active ingredient poorly soluble in water and biopolymers such as hyaluronic acid with a pka-value between 5-7
WO2012085609A1 (en) 2010-12-20 2012-06-28 Dept. Of Pathobiology Treatment of osteoarthritis by continuous intra-articular injection of alginate gel
CA2837558C (en) * 2011-06-02 2018-11-20 Massachusetts Institute Of Technology Modified alginates for cell encapsulation and cell therapy
DE102012208321A1 (en) 2012-05-18 2013-11-21 Robert Bosch Gmbh Alginates as binders for battery cathodes
CN106536606B (en) 2014-05-19 2019-11-08 巴斯夫欧洲公司 The method for preparing the porous aerogel based on alginate
EP3174906A1 (en) 2014-08-01 2017-06-07 Massachusetts Institute Of Technology Modified alginates for anti-fibrotic materials and applications
EP3368085B1 (en) 2015-11-01 2024-01-03 Massachusetts Institute Of Technology Modified alginates for anti-fibrotic materials and applications
CA3027200A1 (en) 2016-06-13 2017-12-21 Massachusetts Institute Of Technology Biocompatible zwitterionic polymer coatings and hydrogels for reducing foreign body response and fibrosis
US11318231B2 (en) 2017-11-06 2022-05-03 Massachusetts Institute Of Technology Anti-inflammatory coatings to improve biocompatibility of neurological implants
US20210015733A1 (en) 2018-04-09 2021-01-21 Basf Se Aerogels and their use in cosmetic applications
CN109646705B (en) * 2019-01-30 2022-06-14 深圳齐康医疗器械有限公司 Composite sponge and preparation method thereof, negative pressure drainage dressing, device and medical equipment
CN110946712B (en) * 2019-12-31 2021-06-18 露乐健康科技股份有限公司 Paper diaper with functions of softening buttocks and building fat
CN111518226A (en) * 2020-03-06 2020-08-11 沈阳科技学院 Preparation method of printing paste for direct printing of reactive dye
CN113208953A (en) * 2021-04-16 2021-08-06 青岛海之林生物科技开发有限公司 Seaweed hair dye cream and preparation process thereof
CN115850533B (en) * 2022-09-28 2023-07-21 青岛格诚经纬生物科技有限公司 Alginic acid material and preparation method and application thereof

Family Cites Families (68)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
CA499026A (en) * 1954-01-05 B. Steiner Arnold Alkylene glycol esters of alginic acid
US2158487A (en) * 1935-10-22 1939-05-16 Kelco Co Triethanolamine alginate product and process
US2426125A (en) * 1944-04-03 1947-08-19 Kelco Co Manufacture of glycol alginates
US2477861A (en) * 1945-11-28 1949-08-02 Donald E Clark Production of fibrous watersoluble alginates
US2494912A (en) * 1947-01-20 1950-01-17 Kelco Co Higher alkylene glycol esters of alginic acid
US2478988A (en) * 1947-03-05 1949-08-16 Walierstein Company Inc Process for improving the foam of fermented malt beverages and product obtained thereby
US2463824A (en) * 1947-08-02 1949-03-08 Kelco Co Substituted alkylene glycol esters of alginic acid
US2647035A (en) * 1951-06-30 1953-07-28 Celanese Corp Dyeing of textile materials using alkylamine alginate thickeners
US2694058A (en) * 1951-10-20 1954-11-09 Hoffmann La Roche Production of polyuronic acid derivatives
US3108042A (en) * 1952-04-07 1963-10-22 Lilly Co Eli Corticotropin reaction complexes
GB768309A (en) * 1954-03-27 1957-02-13 Henkel & Cie Gmbh Process for the production of amides of alginic acid
US2860130A (en) * 1954-11-01 1958-11-11 Kelco Co Methyl alginate
GB833946A (en) * 1957-03-08 1960-05-04 Nordson Pharmaceutical Lab Inc L-amphetamine alginate
US3115488A (en) * 1960-02-29 1963-12-24 American Home Prod Alginic acid methyl ester sulfates, preparation and molecular weight fractionation thereof
US3115458A (en) * 1960-05-11 1963-12-24 Michael J Bebech Apparatus for filtering liquids
GB976301A (en) * 1960-10-27 1964-11-25 Calmic Ltd Preparation and use of alginates
NL273693A (en) * 1961-01-18
US3790558A (en) * 1961-04-24 1974-02-05 Purdue Frederick Co Pyrazolidone derivatives substituted on the 4 position with pectin or algin
US3787389A (en) * 1961-04-24 1974-01-22 Purdue Frederick Co Pyrazolidone derivatives
US3332933A (en) * 1964-02-21 1967-07-25 Kelco Co Diacyl n-alkyl ammonium alginates and their preparation
US3325472A (en) * 1964-06-18 1967-06-13 Mortimer D Sackler Polycyclohexose-polyoxyethyleneglycol suppository bases
US3450814A (en) * 1964-07-15 1969-06-17 Chemway Corp Ophthalmic compositions containing alginic acid salts of pilocarpine,atropine and physostigmine
US3351581A (en) * 1966-06-24 1967-11-07 Kelco Co Acetyl alginates and pectates and process of making the same
US4003792A (en) * 1967-07-01 1977-01-18 Miles Laboratories, Inc. Conjugates of acid polysaccharides and complex organic substances
GB1174854A (en) * 1967-07-07 1969-12-17 Miles Lab New Biologically Active Conjugates
US3535308A (en) * 1968-01-15 1970-10-20 American Cyanamid Co Process for the preparation of partially esterified polyhydroxylic polymers
US3574641A (en) * 1968-03-29 1971-04-13 Kelco Co High neutralized propylene glycol alginate in french dressing
US3967618A (en) * 1969-04-01 1976-07-06 Alza Corporation Drug delivery device
US3993073A (en) * 1969-04-01 1976-11-23 Alza Corporation Novel drug delivery device
DK125598B (en) * 1969-09-29 1973-03-12 Grindstedvaerket As Process for the preparation of propylene glycol alginate.
US3792164A (en) * 1970-03-31 1974-02-12 Chemway Corp Ophthalmic composition comprising water-soluble alkaloid salts of polyuronic acids
GB1355998A (en) * 1970-09-30 1974-06-12 Unilever Ltd Builders for detergent compositions
US3887175A (en) * 1970-11-19 1975-06-03 G A Cochard Lab Quinidine alginate and process of preparation thereof
CA942744A (en) * 1970-12-11 1974-02-26 David J. Pettitt Method for preparing propylene glycol esters of alginic acid
GB1375572A (en) * 1971-08-12 1974-11-27
GB1395898A (en) * 1971-09-28 1975-05-29 Berenguer Beneyto Lab Dihydroquinidine derivative
US4024073A (en) * 1972-01-08 1977-05-17 Toray Industries, Inc. Hydrogel and production thereof
US4206301A (en) * 1972-09-28 1980-06-03 Seymour Yolles Sustained flavor release composition
US3772266A (en) * 1972-10-19 1973-11-13 Kelco Co Process for the preparation of propylene glycol alginate from partially neutralized alginic acid
US4178361A (en) * 1973-09-10 1979-12-11 Union Corporation Sustained release pharmaceutical composition
FR2247204A1 (en) * 1973-10-16 1975-05-09 Girardiere Gf Veterinary aerosol foams - contg alginic acid derivs as film-formers for injection into cows teats, vagina or uterus
US3946110A (en) * 1974-05-30 1976-03-23 Peter, Strong Research And Development Company, Inc. Medicinal compositions and methods of preparing the same
US4002731A (en) * 1974-06-17 1977-01-11 Sterling Drug Inc. Diagnostic process using sodium tyropanoate
CA1019326A (en) * 1974-07-16 1977-10-18 Uniroyal Ltd. Process for the production of alkylene glycol alginates
US4013820A (en) * 1974-11-07 1977-03-22 Abbott Laboratories Universally useable tableting ingredients
CA1057746A (en) * 1975-09-16 1979-07-03 Merck And Co. Propylene glycol alginic acid esters
US4104460A (en) * 1976-09-14 1978-08-01 Nobuyasu Hasebe Method for treating seaweed with hydrogen peroxide or hydrogen peroxide compound
AT358147B (en) * 1976-12-03 1980-08-25 Gergely Gerhard CLEANING MATERIAL
FR2418821A1 (en) * 1978-03-03 1979-09-28 Adeline Andre Continuous mfr. of calcium alginate fibres - by passing calcium chloride and sodium alginate solns. through spinneret
US4330338A (en) * 1978-10-02 1982-05-18 Purdue Research Foundation Pharmaceutical coating composition, and preparation and dosages so coated
US4364929A (en) * 1979-04-02 1982-12-21 The Purdue Frederick Company Germicidal colloidal lubricating gels and method of producing the same
JPS5953951B2 (en) * 1979-04-02 1984-12-27 住友化学工業株式会社 Dyeing method for textile materials
SE442705B (en) * 1979-05-08 1986-01-27 Viktor Kare Larsson Means for forming a protective layer on a substrate in the form of a skin or mucosa and a method for forming a protective layer on the skin for non-therapeutic purposes with the aid of this agent
FR2482603A1 (en) * 1980-05-14 1981-11-20 Pharmindustrie NOVEL HEPARIN ESTERS FOR USE IN THE PREPARATION OF MEDICAMENTS, AND METHODS FOR THEIR PREPARATION
JPS58206751A (en) * 1982-05-26 1983-12-02 日石三菱株式会社 Wound covering material
US4512987A (en) * 1982-07-15 1985-04-23 Ciba-Geigy Corporation New pharmaceutical preparations
US4500676A (en) * 1983-12-15 1985-02-19 Biomatrix, Inc. Hyaluronate modified polymeric articles
JPS60226832A (en) * 1984-04-02 1985-11-12 Daicel Chem Ind Ltd Separating agent containing polysaccharide fatty acid ester
JPH0680081B2 (en) * 1984-04-11 1994-10-12 ダイセル化学工業株式会社 Polysaccharide derivative
JPH0699482B2 (en) * 1984-04-16 1994-12-07 ダイセル化学工業株式会社 Polysaccharide derivative
JPS6130516A (en) * 1984-07-20 1986-02-12 Nichiban Co Ltd Mucosa adhesive pharmaceutical
EP0187703B1 (en) * 1985-01-11 1992-08-05 Teijin Limited Sustained release preparation
US4818751A (en) * 1985-07-02 1989-04-04 Zeria Shinyaku Kogyo Kabushiki Kaisha Cosmetics
US4851521A (en) * 1985-07-08 1989-07-25 Fidia, S.P.A. Esters of hyaluronic acid
GB8519416D0 (en) * 1985-08-01 1985-09-04 Unilever Plc Oligosaccharides
SE452469B (en) * 1986-06-18 1987-11-30 Pharmacia Ab MATERIALS CONSISTING OF A CROSS-BONDED CARBOXYL-GROUPED POLYSACCHARIDE AND PROCEDURE IN THE PREPARATION OF THE SAME
US5147861A (en) * 1986-06-30 1992-09-15 Fidia S.P.A. Esters of alginic acid
US4808707A (en) * 1987-06-08 1989-02-28 University Of Delaware Chitosan alginate capsules

Also Published As

Publication number Publication date
FI872878A0 (en) 1987-06-30
AU602901B2 (en) 1990-11-01
YU46980B (en) 1994-09-09
NO175059B (en) 1994-05-16
EP0251905B1 (en) 1994-11-02
NO872716D0 (en) 1987-06-29
IL82943A (en) 1994-02-27
PL157922B1 (en) 1992-07-31
NO175059C (en) 1994-08-24
ZA874520B (en) 1987-12-29
AU7008491A (en) 1991-05-16
JPH08311104A (en) 1996-11-26
IL82943A0 (en) 1987-12-20
ATE113610T1 (en) 1994-11-15
MX7108A (en) 1994-01-31
PT85200B (en) 1990-03-30
NZ220807A (en) 1992-03-26
IT1203814B (en) 1989-02-23
HUT43870A (en) 1987-12-28
IN166549B (en) 1990-06-02
PH25729A (en) 1991-10-18
EP0609968A3 (en) 1994-12-21
DK333687A (en) 1987-12-31
AR242959A1 (en) 1993-06-30
AU651804B2 (en) 1994-08-04
PL266544A1 (en) 1988-09-15
CN87104499A (en) 1988-04-06
YU46960B (en) 1994-09-09
JP2569054B2 (en) 1997-01-08
NO872716L (en) 1988-01-04
EG18197A (en) 1992-09-30
EP0251905A3 (en) 1988-07-20
DK333687D0 (en) 1987-06-29
DE3750710D1 (en) 1994-12-08
PT85200A (en) 1987-07-01
EP0609968A2 (en) 1994-08-10
EP0251905A2 (en) 1988-01-07
DE3750710T2 (en) 1995-03-16
FI872878A (en) 1987-12-31
JPS6333401A (en) 1988-02-13
CN1026001C (en) 1994-09-28
IT8648201A0 (en) 1986-06-30
YU84688A (en) 1989-10-31
AU7490987A (en) 1988-01-07
HU202559B (en) 1991-03-28
US5336668A (en) 1994-08-09

Similar Documents

Publication Publication Date Title
CA1338235C (en) Esters of alginic acid
US5122598A (en) Polysaccharide esters
US5416205A (en) New esters of alginic acid
EP0265116B1 (en) Cross-linked esters of hyaluronic acid
CA1341276C (en) Hyaluronic acid esters and salts
US5202431A (en) Partial esters of hyaluronic acid
IL90274A (en) Total or partial inter- and intramolecularly esterified hyaluronic acids and their use
US5147861A (en) Esters of alginic acid
US5332809A (en) Partial esters of gellan
CA1338236C (en) Esters of alginic acid
NZ235272A (en) Partial esters of alginic acid and their use in pharmaceuticals, sanitary articles, foods, textiles, printing and paper applications, and detergents

Legal Events

Date Code Title Description
MKLA Lapsed