DE4435652A1 - Coating for bio-material to be used e.g. as sutures - Google Patents

Abstract

A coating for biomaterial which is to be brought into the blood stream or into tissues in the human body consists of a coating material which is compatible with blood and tissue and which inhibits coagulation on the biomaterial caused by the adherence of plasmatic or cellular components. The coating material is a material which is self-adhesive on the biomaterial and forms a varnish-like adhesive layer on the surface of the biomaterial and is permanently degraded in the body, (as described in DE 4334272). The adhesive layer is improved by being of thickness below 100 mu .

Description

The invention relates to a coating for so-called biomaterial according to main patent. . . (Patent application P 43 34 272.8).

A biomaterial is a material that is in the Blood flow or the trade of the human body is introduced, such. B. infusion catheter, cardiac catheter, Balloon catheters, electrodes, sutures for Vascular anastomoses, vascular prostheses or support bodies for vessels, so-called stents, etc., which also temporarily longer term directly in arteries and veins as well as in Body tissues are spent. So serve z. B. the means complicated catheter systems under x-ray control mostly Stents introduced into the coronary arteries after expansion the narrowed area of the artery for internal splinting of the Vessel and remain lifelong for this purpose Job. The dangers to the patient, e.g. B. by Thrombosis and inflammation, are known and with regard to therapy success with the severity of Weigh disease.

After the introduction of biomaterial made of metal and / or various plastics in the bloodstream, e.g. B. at Introducing a catheter can lead to a localized and partially generalized activation of blood clotting come at the biomaterial. It is known that bound Blood plasma proteins, so-called adhesive proteins, such as Albumin, and fibrin films, the adhesion and aggregation of Maintain platelets on the biomaterial. The for the mutual liability of the proteins responsible Peptide structures, the so-called RGD peptides (glycine, Arginine, asparagine) have largely been elucidated. These Structures are also attached to platelet adhesion  corresponding receptors on the platelet surface involved.

Furthermore, biomaterials can be protective Cell layers with which the vessels are lined, and the underlying connective tissue structures, like collagen, expose. Adhesion also takes place there as well as platelet aggregation. At the same time released thromboplastin activates the plasma Coagulation.

The build-up of blood clots on foreign surfaces is hence the consequence of a complex reaction chain more plasmatic and cellular mechanisms of blood clotting, enhanced by Interactions of these systems. If it's through a concomitant drug treatment does not succeed the To completely or partially cancel blood clotting or already Dissolving clots that have formed can result in a cause life-threatening vascular occlusion.

It is also known that blood clots help wound healing trigger by immigrating polyploid stem cells. As a result the excessive growth of so-called "smoother Muscle cells "(smooth muscle cells) can then by caused stenosis of blood flow in the vessels again be restricted.

With the implantation of support bodies for Vessels, the so-called stents, are due to the problems with blood clotting and inflammation many patients only achieved short-term improvements. Through microthrombi at the interface between the vessel wall and Stent can become an undesirable, excessive Vascular proliferation come with renewed narrowing of the vessel. Simultaneous systemic treatment of these patients with high doses of anticoagulant drugs, so-called anticoagulants, such as heparin or Coumarin derivatives is absolutely necessary, partly in  Combination with medication, so-called Antiplatelet drugs that inhibit the Platelets. Also new through the systemic gift developed anticoagulant drugs, such as hirudin, corresponding analogues and newly developed inhibitors Platelet aggregation has the problems associated with the buildup of blood clots on the surfaces of Biomaterials are only marginally improved. The systemic administration of high doses of anticoagulant Medication is at risk of life-threatening bleeding internal organs and the brain connected. Despite the After such interventions, anticoagulation is acute Closures in 4 to 10% of the procedures, restenosis in 35% and threatening bleeding at 5 to 10% clinical Everyday life.

To the accumulation of thrombi on biomaterials, such. B. To prevent catheter surfaces, it is from US Pat. No. 4 281 668 known, biomaterial, in this case a implantable carbon electrode, with a thin Coating of a hydrophilic ion-conducting plastic provided, this plastic of course body, is tissue and / or blood compatible.

Another problem is the germination of Biomaterial. Adsorptively bound proteins of the blood plasma, like albumin, generally the so-called adhesive proteins, and Blood clots provoke the implantation of germs and further the formation of charged slime substances. By these slime-like coatings elude the bacteria the body's defenses and systematically neutralize Antibiotics administered: sensitivity to the Bacteria is drastically reduced. Means intravenous antibiotic therapy can reduce the high bactericidal concentrations cannot always be reached because a dose increase often due to the side effects is contraindicated.  

Only for implants made of biomaterial that are used in the short term Lingering body is due to a rapid removal of the Materials e.g. B. the problem of thrombophlebitis eliminated. As a rule, this does not apply to the medium term or long-term implanted biomaterials. Each Reimplantation is however painful as well as renewed Health hazard burdened.

From US-PS 5 103 837 it is known to be an implanted porous stimulation electrode for a pacemaker a thin coating of a hydrophilic polymer provided, in which an anti-inflammatory steroid is embedded is.

The mentioned and other approaches to solving the problem plasma and cellular blood coagulation and The risk of inflammation essentially affects the change the surface charge, the incorporation of anticoagulant drugs in non-absorbable Plastics or the fixation of drugs by chemical processes. The familiarization and fixation appropriate medicinal substances brought into a plastic matrix but not yet the desired success, because from the immediate layers close to the surface of the drug only released at short notice and in low concentrations will. These surfaces are subsequently in the bloodstream also quickly with protein deposits and blood clots overdrawn. The protein adsorption will release the incorporated or the effect of chemically bound Drugs restricted or even prevented. this leads to a renewed formation of thrombogenic surfaces with the risk of developing blood clots, one excess tissue formation and bacterial colonization.

From DE-PS 39 13 926 is a method for manufacturing known a textile vascular prosthesis. If such textile Vascular prostheses are installed in the human body, they have to be sealed, otherwise through the  Machines of the prosthesis which emits pressurized blood and can cause significant blood loss. These Sealing is carried out according to the mentioned patent a coating with a resorbable plastic, by the entire textile prosthesis with a second one, so to speak Skin around its circumference is completely surrounded. In this However, the patent specification is not an indication of the Prevention of thrombosis included.

WO 84/00302 describes a biocompatible antithrombogenic Known material which, for. B. for the production of artificial skin used in reconstructive surgery becomes. This material consists e.g. B. from polylactide, in the a matrix made of polyurethane is created. This Biodegradable material can be used to make porous Membranes are used to cover large wounds can be. The pores of the material vary depending on Application between 10 and about 100 micrometers (µ) set. However, this material is not used used to coat biomaterial.

The invention has for its object the coating for the biomaterials to be modified so that a Accumulation of blood clots due to plasma or cellular clotting is largely avoided; in addition, it should be possible to also, for. B. anticoagulant or anti-inflammatory agents in the To be able to install the coating, which is also sufficient the surrounding tissue or blood stream are released.

This object is according to the invention by the characterizing part of claim 1 specified Features resolved.

Accordingly, there is the surprisingly simple idea of Invention in biomaterial with a thin, varnish-like Wet coating that in the body, e.g. B. in tissue or is permanently degraded in the bloodstream. The degradation can  hydrolytically and / or enzymatically or by others Decay processes take place. The key here is that the Layer thickness of the degradable or resorbable Coating material smaller than 100 micrometers, in particular less than 50 micrometers or less than 10 Microns are. The layer thicknesses are preferably less than 10 Micrometer. Because of such thin lacquer-like coatings the surface of the biomaterial is practically only wetted, whereas the primary structure of the structure from the Biomaterial is essentially not changed. If accordingly z. B. a porous material, such as the stents mentioned, coated in this way, only the primary structure, hence the strictness of the stent's machine tissue coated, d. H. that generally with porous materials Pores are not closed, only those Primary structure is encased. The porosity remains receive. With such a coating, accordingly porous structure not sealed. For catheters or others Biomaterials with a closed surface are practically only the entire surface is wetted so that there is only a thin one Barrier of about 10 microns and smaller between that Biomaterial and the blood or body tissue created becomes.

For such a paint-like coating with the mentioned small layer thicknesses can only be absorbed materials, e.g. B. plastics are used in volatile Solvents are dissolved, dispersed or emulsified, so that only a coating of the Primary structure of the biomaterial results without the Coating peels off.

Examination results available ex vivo and in vivo have shown that uncoated biomaterials, as already enumerated after only a few minutes of blood contact are covered with a thick blood clot. Already the sole surface coating of these materials with im Body degradable coating materials prevented  through the permanent dismantling processes to a certain extent already the clot adherence. The permanent one Degradation or disintegration of the coating material only allows a temporary liability of the corresponding Blood components such as albumin, adhesive proteins and Platelets etc.

Such materials are suitable for the coating known, some are already delayed under the Release of drugs used in the body. For Achievement of uniform active levels administered enterally Active ingredients have become poorly soluble in the gastrointestinal tract Coatings of capsules, coated tablets, powders or others galenic forms using gelatin, cellulose and (Meth) acrylic acid and its derivatives among others Proven tools. With the development of in the body degradable synthetic polymers used as drug carriers can be used, there are new ways of controlled Release. So today you can look at an extensive Catalog of different materials, which themselves in the structure, the physicochemical properties and distinguish the degradation in the body. The is also known Incorporation of active ingredients into these materials, which then serve as carrier material and the formation of powders, Microspheres and other forms of drugs. After the mostly single subcutaneous intramuscular injection or the Implantation e.g. B. under the skin for a long time thus uniform active level of the incorporated Drugs observed.

Such materials can be used as coating material for the biomaterials in question are used. Preferred as biodegradable coating material Gels, polyglycols or polylactides are used. Exemplary may also be mentioned: biodegradable synthetic polymers, such as polyglycols and polylactides and corresponding Copolymers or mixtures, polyhydroxybutyrates and Polyhydroxyvalerates and corresponding copolymers  and polydioxanone, also starch, gelatin, cellulose, Polyglycolic acid, acrylic acid and methacrylic acid and their Derivatives.

The coating material must be firmly on the surface of the Biomaterials, e.g. B. in the sense of a thin layer of lacquer, adhere to the structure and function of the biomaterial changed. The coating materials are preferred applied to the biomaterial by a dipping process and then dried.

The coating material is preferred as a carrier material used for drugs to be incorporated, so that these Drugs synchronized with the degradation of the carrier material be delivered.

Active substances for inhibiting blood coagulation, preferably two active substances which inhibit or prevent plasma and cellular blood coagulation, are preferably incorporated into the coating material serving as carrier material. After incorporation of such anticoagulant drugs, such. B. hirudin, only very few fibrin threads could be detected on the biomaterial, which were detected using scanning electron microscopy. Comparable findings were made with natural or synthetic prostaglandin derivatives. By combining hirudin with natural or synthetic prostaglandin derivatives, even after prolonged dwelling of the biomaterial in the body with scanning electron microscopy, neither protein deposits or fibrin clots nor aggregated platelets could be detected. Investigations of markers of activated coagulation confirmed these statements. Elevated levels of the thrombin-antithrombin III complexes (TAT complexes) and the prothrombin fragments F _1-2 were only detectable after blood contact with the uncoated materials, but no longer after coating according to the invention. The vascular wall structures that came into direct contact with the coated biomaterials, based on the fine tissue and scanning electron microscopic examinations, do not give any indication of changes in the cell structure of the vascular inner walls. Hyperplasia could not be demonstrated. Even materials made under non-aseptic conditions showed no signs of bacterial colonization after implantation in the femoral artery.

Further improvements could be made by installing anti-adhesive peptides either alone or in combination with the previously mentioned anticoagulant substances or with platelet aggregation inhibitors or with Platelet receptor antagonists can be achieved. Hereby there is the adhesion of the coagulation proteins, the fibrin threads the blood clot and platelets. It then those are missing for the adhesion and aggregation of the Platelets necessary adhesive proteins, which as Bridge proteins act, with the released Antiplatelet agents and / or the Platelet receptor antagonists adhesion and aggregation prevent. The high, local ones Fibrinolytic concentration lyses formed blood clots and lead to continuous self-cleaning of the surfaces.

A possible excess formation of new tissue is indicated by simultaneously existing antiproliferative agents prevented. Corticoids are one of them inflammation-related release of coagulation factors as well prevent from appropriate mediators.

Also the simultaneous use of vasodilators Substances is indicated. It is known that in a Damage to the endothelium endogenous substances that in the normal tissues cause vasodilation, then one bring about a vasoconstricting effect. The local Vascular toning can be achieved by incorporating Nitric oxide (NO) or pharmaceuticals that  Release nitric oxide, such as organic nitrates or Molsidomine, reach into the carrier material.

This makes it possible to have already tried and tested in hospital operation Biomaterials with blood compatible, antiproliferative and to cover antibiotic surfaces, specifically oriented to the needs of the respective patient. Through the continuous self-cleaning of the surfaces at the same time high dosage of locally active drugs become the liability of plasma proteins, training of Coagulation factors and coagulation processes and also the Prevents aggregation of platelets.

By incorporating several active substances against blood coagulation and / or inflammation, synergistic effects are achieved, that are precisely tailored to the respective needs can.

The coating of biomaterial according to the invention can be used for Instruments and devices or the like are used, which are only briefly introduced into the body tissue or into the bloodstream like catheters, sutures etc., but also for Materials that have been in the body for a long time or for life remain so. B. the above-mentioned support body or Stents. Even if after a certain period of time with the help of selected coating material and the coating thickness etc. can be set after some time, e.g. B. some Weeks, the coating material will be completely degraded should, as a rule, no incompatible results Side effects more, because that is what is brought into the body Biomaterial with a body's own tissue or cell layer is provided. From this point on there is also another Blood clotting due to buildup or further inflammation no longer to fear.

The coating material can be applied to the biomaterial in a or applied in several layers, in which case if drugs are incorporated, these drugs  only in one of the layers, in different layers or in all layers can be included. With multilayer Coatings can make up the individual layers different coating materials or Carrier materials exist, which may also be have different rates of degradation. The The layer with the longest dwell time in the body is then in usually arranged as the bottom layer. A drug can then z. B. be incorporated into this layer. The Drugs can also be in the form of powder or crystals Coating material suspended or in the paint-like Surface coating should be homogeneously distributed.

The following are examples of a Surface coating with blood-compatible, antiproliferative, anti-inflammatory and antibiotic Properties mentioned, the active pharmaceutical ingredients in Coating or carrier material suspended and / or are distributed homogeneously.

First, a basic solution for a coating material prepared: 480 mg of a drug carrier, such as poly-D, L-lactide (commercially available as R203 from Boehringer, Ingelheim) in 3 ml chloroform under aseptic conditions solved.

All of the above are suitable for basic solutions biodegradable coating materials in solution, Dispersion or emulsion that is self-adhesive after drying, lacquer-like coatings with the specified thin layer thicknesses surrender.

In this basic solution for the coating or Carrier material can then still sterile active ingredients, such as described below, added to each one to obtain specific coating material.  

For a hirudin coating, 24 mg are finely divided Hirudin powder under aseptic conditions in the Base solution dispersed and until coating at -10 ° C stored. Instead of a hirudin powder, one appropriate drug-containing solution are dispersed; other anticoagulant analogs are also possible Substances such as hirolog. It is also possible that Hirudin powder or other drugs in one to disperse a drug-containing basic solution.

For a coating with a synthetic Prostaglandin derivative (iloprost coating) becomes 0.48 mg Iloprost in aseptic conditions in the basic solution or a corresponding drug-containing solution and stored at -10 ° C until coating.

For a dexamethasone coating, 4.8 mg are fine distributed dexamethasone powder under aseptic conditions in the basic solution or a corresponding one dispersed drug-containing solution and until Coating stored at -10 ° C.

For a gentamicin coating, 4.8 mg are finely divided Gentamicin powder under aseptic conditions in the Basic solution or a corresponding drug-containing Dispersed solution and until coating at -10 ° C stored.

For an EGparin coating, 24 mg are finely divided Heparin powder under aseptic conditions in the Basic solution or a corresponding drug-containing Dispersed solution and until coating at -10 ° C stored.

200,000 units are fine for a urokinase coating distributed urokinase powder under aseptic conditions in the basic solution or a corresponding medicinal product  Dispersed solution and until coating at -10 ° C stored.

The respective biomaterial is used for coating aseptic conditions at about room temperature in the each sticky solution dipped, after which the coated Material is then dried at about 40 ° C. It was found, that with the specified materials actually only that Primary structure of the biomaterial with lacquer-like layers Thicknesses less than 100 microns is wetted, d. H. that the external structure and shape are essentially preserved.

With such solutions, commercially available vascular supports, the so-called stents, vascular prostheses, carbon fiber braids, Pacemaker electrodes, defibrillator electrodes, diagnostic and therapeutic plastic catheters for Angiology and cardiology with and without balloon, tubing and Bags as used in transfusion medicine, Hose systems of heart-lung machines, corresponding Oxigenators, plastic mandrins from Braunülen and Arterial cannulas or sutures for vascular anastomoses coated. The coating adhered to all of these Materials properly and builds up in the bloodstream or in permanently from the tissue in the desired manner. This breakdown was tested in ex vivo and in vivo tests.

The ex vivo test system, as a model of an extracorporeal circuit, consisted of a Braunule for taking blood from the human cubital vein, to which a parallel tube system was connected, which consisted of six approximately five centimeter long pieces of tubing that were made from blood supply lines. Appropriately coated and uncoated biomaterials were introduced into these tubes. Taking blood at the end of each tube ensured that the biomaterials came into contact with blood. Blood could be drawn from each of the tubes depending on the time after blood contact with a syringe. In the blood samples obtained in this way, the investigation of the TAT complexes and the prothrombin fragments F _{1-2 has} proven to be a biochemical marker for activated coagulation. After blood contact, the materials were removed and examined macroscopically and microscopically for the presence of blood clots. A further characterization of any clots was carried out with the aid of scanning electron microscopy, specifically with regard to fibrin deposits and aggregated platelets.

For an in vivo test, e.g. B. plastic mandrins Braunulen or the arterial catheter coated and into the Femoral arteries from non-anticoagulated animals brought in. Uncoated or only served as controls with the degradable coating material in the body coated mandrins. After the trials were completed the materials taken out and macroscopic as well microscopic and scanning electron microscopic Blood clot examined. The one in contact with the mandrins vein walls that have come with the help of the Scanning electron microscopy and various histological Methods for fibrin deposits, aggregated Platelets and tissue reactions of the vessel walls were assessed.

Claims (16)

1. Coating for biomaterial that can be introduced into the blood stream or into the tissue of the human body, the coating consisting of a blood and tissue compatible coating material, by means of which blood coagulation caused by the adherence of plasma or cellular components to the biomaterial is prevented, the coating material is a self-adhesive material on the biomaterial, which forms a lacquer-like adhesive layer on the surface of the biomaterial and is permanently degraded in the body, according to patent (patent application P 43 34 272.8), characterized in that the adhesive layer has a layer thickness of less than 100 micrometers (100 μ ) having. 2. Coating according to claim 1, characterized in that the layer thickness of the lacquer-like layer is less than 50 Micrometer. 3. Coating according to claim 1 or 2, characterized characterized in that the layer thickness of the lacquer-like Layer is less than 10 microns. 4. Coating material according to one of the preceding Claims, characterized in that the Coating material hydrolytically and / or enzymatically and / or permanently through other decay processes is degraded. 5. Coating according to one of the preceding claims, characterized in that as a coating material biodegradable synthetic polymers such as polyglycols and polylactides and corresponding copolymers or mixtures, polyhydroxybutyrates and Polyhydroxyvalerates and corresponding mixed polymers or mixtures, and polydioxanone, also starch,  Gelatin, cellulose, polyglycolic acid, acrylic acid and Methacrylic acid and its derivatives as well as synthetic Polymers are used. 6. Coating according to one of the preceding claims, characterized in that the coating material initially as a solution, dispersion or emulsion in one fast volatile solvent with high Surface tension is present and after application to the Biomaterial and subsequent drying a dry one forms a thin adhesive layer. 7. Coating according to one of the preceding claims, characterized in that in the coating material Drugs are incorporated. 8. Coating according to claim 7, characterized in that inhibiting blood coagulation in the coating material Drugs are incorporated. 9. Coating according to claim 8, characterized in that Drugs to inhibit the plasma and cellular Blood coagulation are incorporated. 10. Coating according to one of claims 7 to 9, characterized characterized in that in the coating material anti-inflammatory drugs are incorporated. 11. Coating according to one of claims 7 to 10, characterized characterized in that in the coating material Antibiotics are incorporated. 12. Coating according to claim 10, characterized in that the anti-inflammatory drugs corticoids contain.   13. Coating according to one of claims 7 to 12, characterized characterized in that in the coating material vasodilatory drugs are incorporated. 14. Coating according to one of the preceding claims, characterized in that several layers of possibly different coating materials are provided are. 15. Coating according to claim 14, characterized in that the layer with the longest dwell time in the body forms the bottom layer. 16. Coating according to one of the preceding claims, characterized in that that to be coated Biomaterial infusion, cardiac or balloon catheter, Vascular prostheses or support bodies for vessels, electrodes for pacemakers and defibrillators as well Suture is.