CA2104045C - Physical trapping type polymeric micelle drug preparation - Google Patents
Physical trapping type polymeric micelle drug preparationInfo
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- CA2104045C CA2104045C CA002104045A CA2104045A CA2104045C CA 2104045 C CA2104045 C CA 2104045C CA 002104045 A CA002104045 A CA 002104045A CA 2104045 A CA2104045 A CA 2104045A CA 2104045 C CA2104045 C CA 2104045C
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- C—CHEMISTRY; METALLURGY
- C08—ORGANIC MACROMOLECULAR COMPOUNDS; THEIR PREPARATION OR CHEMICAL WORKING-UP; COMPOSITIONS BASED THEREON
- C08G—MACROMOLECULAR COMPOUNDS OBTAINED OTHERWISE THAN BY REACTIONS ONLY INVOLVING UNSATURATED CARBON-TO-CARBON BONDS
- C08G69/00—Macromolecular compounds obtained by reactions forming a carboxylic amide link in the main chain of the macromolecule
- C08G69/02—Polyamides derived from amino-carboxylic acids or from polyamines and polycarboxylic acids
- C08G69/08—Polyamides derived from amino-carboxylic acids or from polyamines and polycarboxylic acids derived from amino-carboxylic acids
- C08G69/10—Alpha-amino-carboxylic acids
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- D—TEXTILES; PAPER
- D06—TREATMENT OF TEXTILES OR THE LIKE; LAUNDERING; FLEXIBLE MATERIALS NOT OTHERWISE PROVIDED FOR
- D06F—LAUNDERING, DRYING, IRONING, PRESSING OR FOLDING TEXTILE ARTICLES
- D06F58/00—Domestic laundry dryers
- D06F58/10—Drying cabinets or drying chambers having heating or ventilating means
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- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61K—PREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
- A61K9/00—Medicinal preparations characterised by special physical form
- A61K9/10—Dispersions; Emulsions
- A61K9/107—Emulsions ; Emulsion preconcentrates; Micelles
- A61K9/1075—Microemulsions or submicron emulsions; Preconcentrates or solids thereof; Micelles, e.g. made of phospholipids or block copolymers
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- A—HUMAN NECESSITIES
- A61—MEDICAL OR VETERINARY SCIENCE; HYGIENE
- A61L—METHODS 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
- A61L2/00—Methods or apparatus for disinfecting or sterilising materials or objects other than foodstuffs or contact lenses; Accessories therefor
- A61L2/02—Methods or apparatus for disinfecting or sterilising materials or objects other than foodstuffs or contact lenses; Accessories therefor using physical phenomena
- A61L2/08—Radiation
- A61L2/10—Ultra-violet radiation
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- D06—TREATMENT OF TEXTILES OR THE LIKE; LAUNDERING; FLEXIBLE MATERIALS NOT OTHERWISE PROVIDED FOR
- D06F—LAUNDERING, DRYING, IRONING, PRESSING OR FOLDING TEXTILE ARTICLES
- D06F34/00—Details of control systems for washing machines, washer-dryers or laundry dryers
- D06F34/14—Arrangements for detecting or measuring specific parameters
- D06F34/26—Condition of the drying air, e.g. air humidity or temperature
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- D06F—LAUNDERING, DRYING, IRONING, PRESSING OR FOLDING TEXTILE ARTICLES
- D06F2103/00—Parameters monitored or detected for the control of domestic laundry washing machines, washer-dryers or laundry dryers
- D06F2103/28—Air properties
- D06F2103/32—Temperature
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- D—TEXTILES; PAPER
- D06—TREATMENT OF TEXTILES OR THE LIKE; LAUNDERING; FLEXIBLE MATERIALS NOT OTHERWISE PROVIDED FOR
- D06F—LAUNDERING, DRYING, IRONING, PRESSING OR FOLDING TEXTILE ARTICLES
- D06F2105/00—Systems or parameters controlled or affected by the control systems of washing machines, washer-dryers or laundry dryers
- D06F2105/30—Blowers
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- Y—GENERAL TAGGING OF NEW TECHNOLOGICAL DEVELOPMENTS; GENERAL TAGGING OF CROSS-SECTIONAL TECHNOLOGIES SPANNING OVER SEVERAL SECTIONS OF THE IPC; TECHNICAL SUBJECTS COVERED BY FORMER USPC CROSS-REFERENCE ART COLLECTIONS [XRACs] AND DIGESTS
- Y10—TECHNICAL SUBJECTS COVERED BY FORMER USPC
- Y10T—TECHNICAL SUBJECTS COVERED BY FORMER US CLASSIFICATION
- Y10T428/00—Stock material or miscellaneous articles
- Y10T428/29—Coated or structually defined flake, particle, cell, strand, strand portion, rod, filament, macroscopic fiber or mass thereof
- Y10T428/2982—Particulate matter [e.g., sphere, flake, etc.]
- Y10T428/2984—Microcapsule with fluid core [includes liposome]
- Y10T428/2985—Solid-walled microcapsule from synthetic polymer
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- Y—GENERAL TAGGING OF NEW TECHNOLOGICAL DEVELOPMENTS; GENERAL TAGGING OF CROSS-SECTIONAL TECHNOLOGIES SPANNING OVER SEVERAL SECTIONS OF THE IPC; TECHNICAL SUBJECTS COVERED BY FORMER USPC CROSS-REFERENCE ART COLLECTIONS [XRACs] AND DIGESTS
- Y10—TECHNICAL SUBJECTS COVERED BY FORMER USPC
- Y10T—TECHNICAL SUBJECTS COVERED BY FORMER US CLASSIFICATION
- Y10T428/00—Stock material or miscellaneous articles
- Y10T428/29—Coated or structually defined flake, particle, cell, strand, strand portion, rod, filament, macroscopic fiber or mass thereof
- Y10T428/2982—Particulate matter [e.g., sphere, flake, etc.]
- Y10T428/2989—Microcapsule with solid core [includes liposome]
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Abstract
The present invention relates to drug carriers composed of a block copolymer having hydrophilic and hydrophobic segments, a polymeric micelle type drug comprising hydrophobic drugs trapped by physical treatments in said drug carrier and methods for trapping hydrophobic drugs in the drug carrier. The drugs carrier composed of the block copolymer according to the inven-tion forms a stable polymeric micelle structure with which hydrophobic drugs can be incorporated very efficiently via physical trapping. It was found that the incorporated drug is stably maintained in micelles even in the presence of serum. In addition, a drug difficult to administer into the living body owing to sparing water-solubility for its high hydrophobicity can be administered in the form of polymeric micelle drug.
Description
~10~04~
-PHYSICAL TRAPPING TYPE POLYMERIC MICELLE DRUG PREPARATION
FIELD OF THE INVENTION
The present invention relates to a polymeric micelle type drug containing a hydrophilic drug physically trapped in a drug carrier having hydrophilic and hydrophobic segments as well as to a production process of the polymeric micelle type drug.
BACKGROUND OF THE INVENTION
A polymeric micelle type drug, in which a hydrophobic drug is chemically bound to a block copolymer through a covalent bond, was successfully constructed by the present inventors as described in Unexamined Japanese Patent Publication (Kokai) No. 300,133/1990. In spite of the fact that this prior polymeric micelle type drug is extremely superior as means of administrating a hydrophobic drug, the combination of a hydrophobic drug and a block copolymer is disadvantageously limited because its preparation requires functional groups for chemically binding the hydrophobic drug to the block copolymer.
Under the circumstances, however, no development has been made in a method of physically trapping hydrophobic drugs so as to incorporate them in an inner core of polymeric micelle or in a drug carrier for such a method.
The present inventors have tried to develop a physical trapping type polymeric micelle drug, in order to solve the above disadvantage of the chemical bond type A
210~0~5 polymeric micelle drug. The present inventors, as a result of their eager research, succeeded in preparing a polymeric micelle type drug applicable to a wide variety of combinations of hydrophobic drugs and block copolymer by constructing a polymeric micelle from a drug carrier composed of a block copolymer having hydrophilic and hydrophobic segments and then permitting hydrophobic drugs to be physically trapped into the hydrophobic inner core of said micelle. The syætem for trapping drugs, developed by the present inventors, allows a wide variety of hydrophobic drugs to be easily incorporated in the polymeric micelle.
SUMMARY OF THE INVENTION
The present invention comprises:
1. A polymeric micelle type drug, which comprises a hydrophobic drug physically trapped in a drug carrier composed of a block copolymer represented by the formula I or II:
R1(OCH2CH2)mR2(COCHNH)nR4 Rl(OCH2CH2)mR2(NHCHCO)nR4 II
wherein R1 stands for H or an alkyl group, R2 stands for NH, CO, R6(CH2)qR7 (in which R6 represents OCO, OCONH, NHCO, NHCOO, NHCONH, CONH or COO, R7 represents NH or CO, and q represents 1-6), R3 stands for H, an alkyl group, CH2C6H5, (CH2)pCOOR5 or (CH2)pCONHR5 (in which p represents 1 or 2, R5 represents a C1 20 alkyl group, a benzylsubstituted C1 20 ~10~0~
-alkyl group or a benzyl group), R4 stands for H, OH or an alkyl group carrying CO, NH or O in the terminal, m stands for 4-2500, and n stands for 2-300.
-PHYSICAL TRAPPING TYPE POLYMERIC MICELLE DRUG PREPARATION
FIELD OF THE INVENTION
The present invention relates to a polymeric micelle type drug containing a hydrophilic drug physically trapped in a drug carrier having hydrophilic and hydrophobic segments as well as to a production process of the polymeric micelle type drug.
BACKGROUND OF THE INVENTION
A polymeric micelle type drug, in which a hydrophobic drug is chemically bound to a block copolymer through a covalent bond, was successfully constructed by the present inventors as described in Unexamined Japanese Patent Publication (Kokai) No. 300,133/1990. In spite of the fact that this prior polymeric micelle type drug is extremely superior as means of administrating a hydrophobic drug, the combination of a hydrophobic drug and a block copolymer is disadvantageously limited because its preparation requires functional groups for chemically binding the hydrophobic drug to the block copolymer.
Under the circumstances, however, no development has been made in a method of physically trapping hydrophobic drugs so as to incorporate them in an inner core of polymeric micelle or in a drug carrier for such a method.
The present inventors have tried to develop a physical trapping type polymeric micelle drug, in order to solve the above disadvantage of the chemical bond type A
210~0~5 polymeric micelle drug. The present inventors, as a result of their eager research, succeeded in preparing a polymeric micelle type drug applicable to a wide variety of combinations of hydrophobic drugs and block copolymer by constructing a polymeric micelle from a drug carrier composed of a block copolymer having hydrophilic and hydrophobic segments and then permitting hydrophobic drugs to be physically trapped into the hydrophobic inner core of said micelle. The syætem for trapping drugs, developed by the present inventors, allows a wide variety of hydrophobic drugs to be easily incorporated in the polymeric micelle.
SUMMARY OF THE INVENTION
The present invention comprises:
1. A polymeric micelle type drug, which comprises a hydrophobic drug physically trapped in a drug carrier composed of a block copolymer represented by the formula I or II:
R1(OCH2CH2)mR2(COCHNH)nR4 Rl(OCH2CH2)mR2(NHCHCO)nR4 II
wherein R1 stands for H or an alkyl group, R2 stands for NH, CO, R6(CH2)qR7 (in which R6 represents OCO, OCONH, NHCO, NHCOO, NHCONH, CONH or COO, R7 represents NH or CO, and q represents 1-6), R3 stands for H, an alkyl group, CH2C6H5, (CH2)pCOOR5 or (CH2)pCONHR5 (in which p represents 1 or 2, R5 represents a C1 20 alkyl group, a benzylsubstituted C1 20 ~10~0~
-alkyl group or a benzyl group), R4 stands for H, OH or an alkyl group carrying CO, NH or O in the terminal, m stands for 4-2500, and n stands for 2-300.
2. The drug according to 1, in which the block copolymer is a compound represented by formula III:
CH3--~ CK~H~C~h~n~ CXX~HNE~H
C~I ~ 2 ~ m wherein m stands for 4-2500 and n stands for 2-300.
CH3--~ CK~H~C~h~n~ CXX~HNE~H
C~I ~ 2 ~ m wherein m stands for 4-2500 and n stands for 2-300.
3. The drug according to 1, in which the hydrophobic drug i5 adriamycin or indomethacin.
4. The drug according to 1, in which the hydrophobic drug is adriamycin, and the block copolymer is a compound of formula III.
5. The drug according to 1, in which the hydrophobic drug is indomethacin, and the block copolymer is a compound of formula III.
6. A method for producing the polymeric micelle type drug mentioned above, which comprises heating, ultra-sonication or organic solvent treatment of the hydrophobic drug and a drug carrier of formula I, II or III to A~
physically trap said hydrophobic drugs in polymeric micelles composed of said drug carrier.
BRIEF DESCRIPTION OF THE DRAWINGS
FIG. 1 shows particle size distribution by dynamic light scattering of polymeric micelles of polyethylene oxide-poly-(~-benzyl L-aspartate) block copolymer (A-5-10) in an aqueous solution.
FIG. 2 shows changes in florescence spectra of pyrene when incorporated in the inner core of polymeric micelle by heating.
In the figure, Nos. 1-8 indicate the fluorescence spectra of pyrene at the respective concentrations of block copolymer.
FIG. 3 shows the amount of pyrene incorporated by three methods at various concentrations of block copolymer.
FIG. 4 is a gel permeation chromatogram (GPC) of adriamycin incorporated into polymeric micelles.
FIG. 5 is a gel permeation chromatogram of polymeric mi-celles.
FIG. 6 is a gel permeation chromatogram of adriamycin incorporated in micelles after allowed to stand for 5 hours in the presence of 50~(V/V) of fetal bovine serum.
FIG. 7 is a gel permeation chromatogram of 50%(V/V) fetal bovine serum.
FIG. 8 is a gel permeation chromatogram monitored at 312 nm at 210~045 .
which indomethacin shows characteriætic absorption.
DETAILED DESCRIPTION OF THE INVENTION
The hydrophilic segment of the block copolymeremployed according to the invention is derived from polyethylene oxide or its alkyl ether derivative. Other materials that could be used as the hydrophilic segment include polyalkylene oxides, polymalic acid, polyaspartic acid, polyglutamic acid, polylysine, polysaccharide, polyacrylamide, polyacrylic acid, polymethacrylamide, polymethacrylic acid, polyvinyl pyrrolidone, polyvinyl alcohol, polymethacrylate, polyacrylate, polyamino acids and segments derived from derivatives thereof.
The hydrophobic segment of the block copolymer employed according to the invention includes e.g. poly(~-benzyl L-aspartate), poly(~-benzyl L-glutamate), poly(~-substituted aspartate), poly(y-substituted glutamate), poly(L-leucine), poly(L-valine), poly(L-phenylalanine) and other hydrophobic polyamino acids. Other materials that could be used as the hydrophobic segment includes polystyrene, polymethacrylate, polyacrylate, polymethacrylate amide, polyacrylate amide, polyamide, polyester, polyalkylene oxide and hydrophobic polyolefins.
Examples of the block copolymer consisting of hydrophilic and hydrophobic segments that could be used according to the present invention include polyethylene oxide-polystyrene block copolymer, polyethylene oxide-polybutadiene block copolymer, polyethylene oxide-210~04~
polyisoprene block copolymer, polyethylene oxide-polypropylene block copolymer, polyethylene oxide-polyethylene block copolymer, polyethylene oxide-5a ~104û45 poly(~-benzylaspartate) block copolymer, polyethylene oxide-poly(r-benzylglutamate) block copolymer, polyethylene oxide-poly(alanine) block copolymer, polyethylene oxide-poly(phenylalanine) block copolymer, polyethylene oxide-poly(leucine) block copolymer, polyethylene oxide-poly(isoleu-cine) block copolymer, polyethylene oxide-poly(valine) block copolymer, polyacrylic acid-polystyrene block copolymer, polyacrylic acid-polybutadiene block copolymer, polyacrylic acid-polyisoprene block copolymer, polyacrylic acid-polyprop-ylene block copolymer, polyacrylic acid-polyethylene block copolymer, polyacrylic acid-poly(~-benzylaspartate) block copolymer, polyacrylic acid-poly(r-benzylglutamate) block copolymer, polyacrylic acid-poly(alanine)block copolymer, polyacrylic acid-poly(phenylalanine) block copolymer, polyac-rylic acid-poly(leucine) block copolymer, polyacrylic acid-poly(isoleucine) block copolymer, polyacrylic acid-poly(valine)block copolymer, polymethacrylic acid-polyst-yrene block copolymer, polymethacrylic acid-polybutadiene block copolymer, polymethacrylic acid-polyisoprene block copolymer, polymethacrylic acid-polypropyleneblockcopoIymer, polymethac-rylic acid-polyethylene block copolymer, polymethacrylic acid-poly(~-benzylaspartate) block copolymer, polymethacrylic acid-poly(r-benzyl glutamate) block copolymer, polymethacrylic acid-poly(alanine)blockcopolymer,polymethacrylicacid-poly(p-21~4045 henylalanine) block copolymer, polymethacrylic acid-poly(leu-cine) block copolymer, polymethacrylic acid-poly(isoleucine) block copolymer, polymethacrylic acid-poly(valine) block copolymer, poly(N-vinylpyrrolidone)-polystyrene block copolymer, poly(N-vinylpyrrolidone)-polybutadiene block copolymer, poly(N-vinylpyrrolidone)-polyisoprene block copolymer, poly(N-vinylpyrrolidone)-polypropylene block copolymer, poly(N-vinylpyrrolidone)-polyethylene block copolymer, poly(N-vinylpyrrolidone)-poly(~-benzylaspartate) block copolymer, poly(N-vinylpyrrolidone)-poly(7-benzylglutamate) block copolymer, poly(N-vinylpyrrolidone)-poly(alanine) block copolymer, poly(N-vinylpyrrolidone)-poly(phenylalanine) block copolymer, poly(N-vinylpyrrolidone)-poly(leucine) block copolymer, poly(N-vinylpyrrolidone)-poly(isoleucine) block copolymer, poly(N-vinylpyrrolidone)-poly(valine) block copolymer, poly(aspartic acid)-polystyrene block copolymer, poly(asparticacid)-polybutadieneblockcopolymer,poly(aspartic acid)-polyisoprene block copolymer, poly(aspartic acid)-polypropylene block copolymer, poly(aspartic acid) polyethylene block copolymer, poly(aspartic acid)-poly(~-benzylaspartate) block copolymer, poly(aspartic acid)-poly(r-benzylglutamate) block copolymer, poly(aspartic acid)-poly(alanine) block copolymer, poly(aspartic acid)--poly(phenylalanine) block copolymer, poly(aspartic acid)-- 21Q40~
-poly(leucine) block copolymer, poly(aspartic acid)-poly(isoleucine) block copolymer, poly(aspartic acid)-poly(valine) block copolymer, poly(glutamic acid)-polystyrene block copolymer, poly(glutamic acid)-polybutadiene block copolymer, poly(glutamic acid)-polyisoprene block copolymer, poly(glutamicacid)-polypropyleneblockcopolymer,poly(glutamic acid)-polyethylene block copolymer, poly(glutamic acid)-poly(~-benzylaspartate) block copolymer, poly(glutamic acid)-poly(~-benzylglutamate) block copolymer, poly(glutamic acid)-poly(alanine) block copolymer, poly(glutamic acid)-poly(phenylalanine) block copolymer, poly(glutamic acid)-poly(leucine) block copolymer, poly(glutamic acid)-poly(isoleucine) block copolymer and poly(glutamic acid)-poly(valine) block copolymer.
The drug to be physically trapped in the hydrophobic inner core of polymeric micelle is not particularly limited. Examples are anticancer drugs such as adriamycin, daunomycin, methotrex-ate, mitomycin C, etc., painkilling and anti-inflammatory drugs such as indomethacin etc., drugs for the central nervous system, drugs fortheperipheral nervoussystem, drugsagainst allergies, drugs for the circulatory organs, drugs for the respiratory organs, drugs for the digestive organs, hormones as drugs, metabolizing drugs, antibiotics, drugs for use in chemotherapy, etc.
The physicalmeàns oftrapping hydrophobicdrugs in polymeric 210~045 micelles composed of the present drug carrier includes heating, ultrasonication and organic solvent treatment, which are conducted solely or in combination with one another.
Heating is carried out at 30-100C for a period of time from 10 min. to 24 hours. Ultrasonication is carried out in the range of 1-200 W for a period of time from 1 second to 2 hours. The organic solvent used in organic solvent treatment iæ DMF, DMSO, dioxane, chloroform, n-hexane, toluene, methylene chloride, etc., which is used in the absence of water or after added in an amount of 0.01 % (vtv) or more to water.
Hereinafter, the present invention is specifically explained in detail with reference to the actual incorporation of adriamycin as an anticancer drug, indomethacin as a painkilling, anti-inflammatory drug and pyrene as a typical hydrophobic chemical, into an AB type block copolymer composed of a hydrophilic segment derived from a derivative of polyethylene oxide and a hydrophobic segment of poly(~-benzyl L-aspartate).
The compound of the formula:
CH3--~CK~H2C~khn~ t CXX~1NHhrH
CEkCrKXoH2 ~
A
21040~5 -is polyethylene oxide-poly(~-benzyl L-aspartateJblock copolymer consisting of polyethylene oxide and poly(~-benzyl L-aspartate) which have hydrophilic and hydrophobic properties, respectively.
9a 21~0~5 The compound of formula IV is compound of formula I wherein R1is a methyl group, Rz is NH, R3 is CH2COOCHzC6Hs, and R4 is H.
This block copolymer is prepared by polymerizing, in the presence of an initiator, ~-benzyl L-aspartate N-carboxy anhydride from the terminal primary amino group of polyethylene oxide (molecular weight of 200-250,000) having an amino group in one terminal and a methoxy group at the other terminal. The portion of poly(~-benzyl L-aspartate) in the block copolymer polyethylene oxide-poly(~-benzyl L-aspartate) may have a molecular weight varying from 205 to 62,000. By suitable selection of a chain length ratio of the two segments, this block copolymer forms a polymeric micelle with ethylene oxide as an outer shell and poly(~-benzyl L-aspartate) as an inner core.
Thispolymericmicellecanstablyincorporatehydrophobicpyrene, adriamycin and indomethacin by heating, ultrasonication, or treatment with organic solvent.
The drug carrier composed of the block copolymer according to the invention forms a stable polymeric micelle structure with which hydrophobic drugs can be incorporated very efficiently via physical trapping into the inner core. A drug difficult to administerinto the livingbodyowingto sparing water-solubility for its high hydrophobicity can be administered in the form of polymeric micelle type drug.
In addition, the invention do not require any functional - 2104~4~
group for chemical bonding and thereby enables a wide variety of combinations of hydrophobic drugs and polymeric micelle.
EXAMPLES
The present invention is described in detail with reference to the following examples, which however are not intended to limit the scope of the invention.
Example 1 ~ -benzyl L-aspartate N-carboxylic anhydride (1.99 g) was dissolved in 3 ml N,N-dimethylformamide, followed by addition of 15 ml of chloroform. Separately, 4.00 g of polyethylene oxide having methoxy group in one terminal and an amino group in the other terminal (molecular weight: 5,000) was dissolved in 15 ml chloroform, and the solution was then added to the above solution of ~-benzyl L-aspartate N-carboxy anhydride. 26 hours thereaf-ter, the reaction mixture was added dropwise to 330 ml diethyl ether, thereby giving rise to polymer precipitates which in turn were recovered by filtration, then washed with diethyl ether and dried under vacuum, to give polyethylene oxide poly(~-benzyl L-aspartate) block copolymer (referred to as "PEO-PBLA,"
hereinafter)(A-5-10). Yield was 5.13 g(91 %). The compositions of block copolymers thus synthesized are summarized in Table 1.
210~ 5 Table 1 - ~~ Characterization of Polyethylene Oxide-Poly(~-Benzyl L-Aspartate) Block Copolymer and Micelles Pa~icle Sampie PE0 wt(?') ' ~n' n?E0 npBLA' size(mm)b C`,~C(!n~/L) A-5-10 l3. 07000 ii0 9. 0 !8 10 A-~-20 53. 39100 110 19 11 5. 0 A-12-20 35. 016000 270 20 21 10 a) determined by 1H-NMR
b) determined by dynamic light scattering (number-avarage) Example 2 Formation of Micelles The block copolymer synthesized in Example 1 was dissolved at a concentration of 0.01-0.1 %(w/v)in wateror asuitable buffer.
The formation of micelles in the thus obtained solutions was ascertained by measurement.of distribution of particle size by dynamic light scattering. The result is set forth in FIG. 1. The particle size of micelle and critical micelle concentration are also shown in Table 1.
Example 3 Incorporation of Pyrene into Micelles Pyrene of formula V:
~ V
is sparingly soluble in water so that a predetermined amount of pyrene was dissolved at acetone. After dissolved, acetone was removed under a nitrogen atmosphere, and a micelle solution of PE0-PBLA (A-5-lO)in distilled water was added at a concentration shown in Table 1 to the pyrene.
1. Incorporation by Stirring The above mixture was stirred for 2 days so that pyrene was incorporated into micelles.
2. Incorporation by Heating The above mixture was heated at 80 C for 2 hours so that pyrene was incorporated into micelles.
3. Incorporation by Ultrasonication The above mixture was ultrasonicated for 15 seconds so that pyrene was incorporated into micelles.
4. Incorporation by Treatment with DMF for Making the PBLA
segment swelled in the PE0-PBLA micelle.
As described above, acetone was removed from the pyrene solution. To the pyrene was added DMF in an amount of 30 %
relative to the micelle solution to be added afterward. Then, a solution of PE0-PBLA in distilled water was then added in a concentration shown in Table 3 to the pyrene solution. After stirred for 15 hours, the solution was dialyzed in a dialysis tube Spectrapor 6 (cut off molecular weight = 1,000) against water.
21~ 5 According to the above procedure, pyrene was incorporated into micelles.
As is evident from increases in the intensities of the fluorescence spectra of the heated sample shown in FIG. 2, the incorporation of pyrene into micelles was confirmed in every incorporation means. FIG. 3 shows a comparison between the amounts of pyrene incorporated into micelles, where the lncorpo-ration means by heating attains theamount of incorporated pyrene as approx. 250 times high as the amount of pyrene saturated in water. Table 2 shows the partition coefficient of pyrene into PE0-PBLA (A-5-10) micelle relative to water.
Table 2 . Distribution Coefficient into Micelle Solution of Polyethylene Oxide-Poly(~-Benzyl L-Aspartate) Block Copolymer Means of Incorporating Pyrene Distribution Coefficient (Kn) Stirring 17000 Heating at 80 C 21000 Ultrasonication 17000 Example 4 5 mg of adriamycin hydrochloride and 5 mg of PE0-PBLA
(A-12-20) were added to 5 ml of 0.1 M Tris buffer, pH 9.1. Then, adriamycin was made miscible into micelles by stirring and ultrasonication.
Adriamycin is the compound of the following formula:
21040~
--- O OH
~COCH20H
CH O OH `o ~H3 , NH~
This compound itself does not dissolve in Tris buffer, pH 9.1, but can be completely dissolved according to the above procedure.
As shown in FIG. 4, adriamycin appeared in gel-exclusion volume in GPC where the sample was monitored at 485 nm at which adria-mycin shows characteristic absorption, and this indicates sufficient incorporation of adriamycin into micelles. In FIG. 4, elution volume is indicated as numerical values where 1.792, 3.292 and 9.300 mean micelles, a single polymer and unincorpo-rated adriamycin, respectively.
Example 5 4.4 ~11 triethylamine and 20 mg PE0-PBLA block copolymer (A-12-20) were added to a solution of 14 mg adriamycin hydrochlo-ride in 4 ml DMF, and the mixture was stirred for 10 min. and then dialyzed for 15 hours against distilled water. Dynamic light scattering indicated that the sample thus obtained formed polymeric micelles with a weight-average diameter of 55 nm. FIG.
5 shows a gel permeation chromatogram of the polymeric micelles monitored at 485 nm. Adriamycin was incorporated in the 21040~5 m~celles, as can be seen from its elution as micelles in gel exclusion volume (4.2-4.3 ml). FIG. 6 shows a gel permeation chromatogramofadriamycinincorporatedinmicellesafterallowed to stand for 5 hours in the presence of 50%(V/V) fetal bovine serum. In FIG. 6, the peak (4.25 ml) eluted in gel exclusion volume and not present in the serum itself was not lowered in the presence of serum (Fig. 7), which indicates that adriamycin can be stably maintained in micells even in the presence of serum.
Example 6 15 mg of indomethacin of formula CO -~ Cl ~N\~CH3 V~
CH30~ CH2COOH
as an anti-inflammatory drug was dissolved in 4 ml DMF, followed by addition of 20 mg of PE0-PBLA block copolymer (A-12-20). The mixture was stirred for 15 hours and dialyzed for 3 hours against 0.1 M phosphate buffer, pH 7.4, and then against water for 6 hours. The resulting sample was found to form polymric micelles with a weight-average diameter of 56 nm, as determined by dynamic light scattering. FIG. 8 shows a gel permeation chromatogram monitored at 312 nm at which indomethacin shows characteristic 21040~
absorption. The indomethacin was eluted as micelles in gel exclusion volume, indicating the incorporation of the indometha-cin into micelles. 0.76 mg of indomethacin was found to be incorporated in the micelles from its adsorption monitored at 312 nm in a solvent of DMF/distilled water (7: 3).
physically trap said hydrophobic drugs in polymeric micelles composed of said drug carrier.
BRIEF DESCRIPTION OF THE DRAWINGS
FIG. 1 shows particle size distribution by dynamic light scattering of polymeric micelles of polyethylene oxide-poly-(~-benzyl L-aspartate) block copolymer (A-5-10) in an aqueous solution.
FIG. 2 shows changes in florescence spectra of pyrene when incorporated in the inner core of polymeric micelle by heating.
In the figure, Nos. 1-8 indicate the fluorescence spectra of pyrene at the respective concentrations of block copolymer.
FIG. 3 shows the amount of pyrene incorporated by three methods at various concentrations of block copolymer.
FIG. 4 is a gel permeation chromatogram (GPC) of adriamycin incorporated into polymeric micelles.
FIG. 5 is a gel permeation chromatogram of polymeric mi-celles.
FIG. 6 is a gel permeation chromatogram of adriamycin incorporated in micelles after allowed to stand for 5 hours in the presence of 50~(V/V) of fetal bovine serum.
FIG. 7 is a gel permeation chromatogram of 50%(V/V) fetal bovine serum.
FIG. 8 is a gel permeation chromatogram monitored at 312 nm at 210~045 .
which indomethacin shows characteriætic absorption.
DETAILED DESCRIPTION OF THE INVENTION
The hydrophilic segment of the block copolymeremployed according to the invention is derived from polyethylene oxide or its alkyl ether derivative. Other materials that could be used as the hydrophilic segment include polyalkylene oxides, polymalic acid, polyaspartic acid, polyglutamic acid, polylysine, polysaccharide, polyacrylamide, polyacrylic acid, polymethacrylamide, polymethacrylic acid, polyvinyl pyrrolidone, polyvinyl alcohol, polymethacrylate, polyacrylate, polyamino acids and segments derived from derivatives thereof.
The hydrophobic segment of the block copolymer employed according to the invention includes e.g. poly(~-benzyl L-aspartate), poly(~-benzyl L-glutamate), poly(~-substituted aspartate), poly(y-substituted glutamate), poly(L-leucine), poly(L-valine), poly(L-phenylalanine) and other hydrophobic polyamino acids. Other materials that could be used as the hydrophobic segment includes polystyrene, polymethacrylate, polyacrylate, polymethacrylate amide, polyacrylate amide, polyamide, polyester, polyalkylene oxide and hydrophobic polyolefins.
Examples of the block copolymer consisting of hydrophilic and hydrophobic segments that could be used according to the present invention include polyethylene oxide-polystyrene block copolymer, polyethylene oxide-polybutadiene block copolymer, polyethylene oxide-210~04~
polyisoprene block copolymer, polyethylene oxide-polypropylene block copolymer, polyethylene oxide-polyethylene block copolymer, polyethylene oxide-5a ~104û45 poly(~-benzylaspartate) block copolymer, polyethylene oxide-poly(r-benzylglutamate) block copolymer, polyethylene oxide-poly(alanine) block copolymer, polyethylene oxide-poly(phenylalanine) block copolymer, polyethylene oxide-poly(leucine) block copolymer, polyethylene oxide-poly(isoleu-cine) block copolymer, polyethylene oxide-poly(valine) block copolymer, polyacrylic acid-polystyrene block copolymer, polyacrylic acid-polybutadiene block copolymer, polyacrylic acid-polyisoprene block copolymer, polyacrylic acid-polyprop-ylene block copolymer, polyacrylic acid-polyethylene block copolymer, polyacrylic acid-poly(~-benzylaspartate) block copolymer, polyacrylic acid-poly(r-benzylglutamate) block copolymer, polyacrylic acid-poly(alanine)block copolymer, polyacrylic acid-poly(phenylalanine) block copolymer, polyac-rylic acid-poly(leucine) block copolymer, polyacrylic acid-poly(isoleucine) block copolymer, polyacrylic acid-poly(valine)block copolymer, polymethacrylic acid-polyst-yrene block copolymer, polymethacrylic acid-polybutadiene block copolymer, polymethacrylic acid-polyisoprene block copolymer, polymethacrylic acid-polypropyleneblockcopoIymer, polymethac-rylic acid-polyethylene block copolymer, polymethacrylic acid-poly(~-benzylaspartate) block copolymer, polymethacrylic acid-poly(r-benzyl glutamate) block copolymer, polymethacrylic acid-poly(alanine)blockcopolymer,polymethacrylicacid-poly(p-21~4045 henylalanine) block copolymer, polymethacrylic acid-poly(leu-cine) block copolymer, polymethacrylic acid-poly(isoleucine) block copolymer, polymethacrylic acid-poly(valine) block copolymer, poly(N-vinylpyrrolidone)-polystyrene block copolymer, poly(N-vinylpyrrolidone)-polybutadiene block copolymer, poly(N-vinylpyrrolidone)-polyisoprene block copolymer, poly(N-vinylpyrrolidone)-polypropylene block copolymer, poly(N-vinylpyrrolidone)-polyethylene block copolymer, poly(N-vinylpyrrolidone)-poly(~-benzylaspartate) block copolymer, poly(N-vinylpyrrolidone)-poly(7-benzylglutamate) block copolymer, poly(N-vinylpyrrolidone)-poly(alanine) block copolymer, poly(N-vinylpyrrolidone)-poly(phenylalanine) block copolymer, poly(N-vinylpyrrolidone)-poly(leucine) block copolymer, poly(N-vinylpyrrolidone)-poly(isoleucine) block copolymer, poly(N-vinylpyrrolidone)-poly(valine) block copolymer, poly(aspartic acid)-polystyrene block copolymer, poly(asparticacid)-polybutadieneblockcopolymer,poly(aspartic acid)-polyisoprene block copolymer, poly(aspartic acid)-polypropylene block copolymer, poly(aspartic acid) polyethylene block copolymer, poly(aspartic acid)-poly(~-benzylaspartate) block copolymer, poly(aspartic acid)-poly(r-benzylglutamate) block copolymer, poly(aspartic acid)-poly(alanine) block copolymer, poly(aspartic acid)--poly(phenylalanine) block copolymer, poly(aspartic acid)-- 21Q40~
-poly(leucine) block copolymer, poly(aspartic acid)-poly(isoleucine) block copolymer, poly(aspartic acid)-poly(valine) block copolymer, poly(glutamic acid)-polystyrene block copolymer, poly(glutamic acid)-polybutadiene block copolymer, poly(glutamic acid)-polyisoprene block copolymer, poly(glutamicacid)-polypropyleneblockcopolymer,poly(glutamic acid)-polyethylene block copolymer, poly(glutamic acid)-poly(~-benzylaspartate) block copolymer, poly(glutamic acid)-poly(~-benzylglutamate) block copolymer, poly(glutamic acid)-poly(alanine) block copolymer, poly(glutamic acid)-poly(phenylalanine) block copolymer, poly(glutamic acid)-poly(leucine) block copolymer, poly(glutamic acid)-poly(isoleucine) block copolymer and poly(glutamic acid)-poly(valine) block copolymer.
The drug to be physically trapped in the hydrophobic inner core of polymeric micelle is not particularly limited. Examples are anticancer drugs such as adriamycin, daunomycin, methotrex-ate, mitomycin C, etc., painkilling and anti-inflammatory drugs such as indomethacin etc., drugs for the central nervous system, drugs fortheperipheral nervoussystem, drugsagainst allergies, drugs for the circulatory organs, drugs for the respiratory organs, drugs for the digestive organs, hormones as drugs, metabolizing drugs, antibiotics, drugs for use in chemotherapy, etc.
The physicalmeàns oftrapping hydrophobicdrugs in polymeric 210~045 micelles composed of the present drug carrier includes heating, ultrasonication and organic solvent treatment, which are conducted solely or in combination with one another.
Heating is carried out at 30-100C for a period of time from 10 min. to 24 hours. Ultrasonication is carried out in the range of 1-200 W for a period of time from 1 second to 2 hours. The organic solvent used in organic solvent treatment iæ DMF, DMSO, dioxane, chloroform, n-hexane, toluene, methylene chloride, etc., which is used in the absence of water or after added in an amount of 0.01 % (vtv) or more to water.
Hereinafter, the present invention is specifically explained in detail with reference to the actual incorporation of adriamycin as an anticancer drug, indomethacin as a painkilling, anti-inflammatory drug and pyrene as a typical hydrophobic chemical, into an AB type block copolymer composed of a hydrophilic segment derived from a derivative of polyethylene oxide and a hydrophobic segment of poly(~-benzyl L-aspartate).
The compound of the formula:
CH3--~CK~H2C~khn~ t CXX~1NHhrH
CEkCrKXoH2 ~
A
21040~5 -is polyethylene oxide-poly(~-benzyl L-aspartateJblock copolymer consisting of polyethylene oxide and poly(~-benzyl L-aspartate) which have hydrophilic and hydrophobic properties, respectively.
9a 21~0~5 The compound of formula IV is compound of formula I wherein R1is a methyl group, Rz is NH, R3 is CH2COOCHzC6Hs, and R4 is H.
This block copolymer is prepared by polymerizing, in the presence of an initiator, ~-benzyl L-aspartate N-carboxy anhydride from the terminal primary amino group of polyethylene oxide (molecular weight of 200-250,000) having an amino group in one terminal and a methoxy group at the other terminal. The portion of poly(~-benzyl L-aspartate) in the block copolymer polyethylene oxide-poly(~-benzyl L-aspartate) may have a molecular weight varying from 205 to 62,000. By suitable selection of a chain length ratio of the two segments, this block copolymer forms a polymeric micelle with ethylene oxide as an outer shell and poly(~-benzyl L-aspartate) as an inner core.
Thispolymericmicellecanstablyincorporatehydrophobicpyrene, adriamycin and indomethacin by heating, ultrasonication, or treatment with organic solvent.
The drug carrier composed of the block copolymer according to the invention forms a stable polymeric micelle structure with which hydrophobic drugs can be incorporated very efficiently via physical trapping into the inner core. A drug difficult to administerinto the livingbodyowingto sparing water-solubility for its high hydrophobicity can be administered in the form of polymeric micelle type drug.
In addition, the invention do not require any functional - 2104~4~
group for chemical bonding and thereby enables a wide variety of combinations of hydrophobic drugs and polymeric micelle.
EXAMPLES
The present invention is described in detail with reference to the following examples, which however are not intended to limit the scope of the invention.
Example 1 ~ -benzyl L-aspartate N-carboxylic anhydride (1.99 g) was dissolved in 3 ml N,N-dimethylformamide, followed by addition of 15 ml of chloroform. Separately, 4.00 g of polyethylene oxide having methoxy group in one terminal and an amino group in the other terminal (molecular weight: 5,000) was dissolved in 15 ml chloroform, and the solution was then added to the above solution of ~-benzyl L-aspartate N-carboxy anhydride. 26 hours thereaf-ter, the reaction mixture was added dropwise to 330 ml diethyl ether, thereby giving rise to polymer precipitates which in turn were recovered by filtration, then washed with diethyl ether and dried under vacuum, to give polyethylene oxide poly(~-benzyl L-aspartate) block copolymer (referred to as "PEO-PBLA,"
hereinafter)(A-5-10). Yield was 5.13 g(91 %). The compositions of block copolymers thus synthesized are summarized in Table 1.
210~ 5 Table 1 - ~~ Characterization of Polyethylene Oxide-Poly(~-Benzyl L-Aspartate) Block Copolymer and Micelles Pa~icle Sampie PE0 wt(?') ' ~n' n?E0 npBLA' size(mm)b C`,~C(!n~/L) A-5-10 l3. 07000 ii0 9. 0 !8 10 A-~-20 53. 39100 110 19 11 5. 0 A-12-20 35. 016000 270 20 21 10 a) determined by 1H-NMR
b) determined by dynamic light scattering (number-avarage) Example 2 Formation of Micelles The block copolymer synthesized in Example 1 was dissolved at a concentration of 0.01-0.1 %(w/v)in wateror asuitable buffer.
The formation of micelles in the thus obtained solutions was ascertained by measurement.of distribution of particle size by dynamic light scattering. The result is set forth in FIG. 1. The particle size of micelle and critical micelle concentration are also shown in Table 1.
Example 3 Incorporation of Pyrene into Micelles Pyrene of formula V:
~ V
is sparingly soluble in water so that a predetermined amount of pyrene was dissolved at acetone. After dissolved, acetone was removed under a nitrogen atmosphere, and a micelle solution of PE0-PBLA (A-5-lO)in distilled water was added at a concentration shown in Table 1 to the pyrene.
1. Incorporation by Stirring The above mixture was stirred for 2 days so that pyrene was incorporated into micelles.
2. Incorporation by Heating The above mixture was heated at 80 C for 2 hours so that pyrene was incorporated into micelles.
3. Incorporation by Ultrasonication The above mixture was ultrasonicated for 15 seconds so that pyrene was incorporated into micelles.
4. Incorporation by Treatment with DMF for Making the PBLA
segment swelled in the PE0-PBLA micelle.
As described above, acetone was removed from the pyrene solution. To the pyrene was added DMF in an amount of 30 %
relative to the micelle solution to be added afterward. Then, a solution of PE0-PBLA in distilled water was then added in a concentration shown in Table 3 to the pyrene solution. After stirred for 15 hours, the solution was dialyzed in a dialysis tube Spectrapor 6 (cut off molecular weight = 1,000) against water.
21~ 5 According to the above procedure, pyrene was incorporated into micelles.
As is evident from increases in the intensities of the fluorescence spectra of the heated sample shown in FIG. 2, the incorporation of pyrene into micelles was confirmed in every incorporation means. FIG. 3 shows a comparison between the amounts of pyrene incorporated into micelles, where the lncorpo-ration means by heating attains theamount of incorporated pyrene as approx. 250 times high as the amount of pyrene saturated in water. Table 2 shows the partition coefficient of pyrene into PE0-PBLA (A-5-10) micelle relative to water.
Table 2 . Distribution Coefficient into Micelle Solution of Polyethylene Oxide-Poly(~-Benzyl L-Aspartate) Block Copolymer Means of Incorporating Pyrene Distribution Coefficient (Kn) Stirring 17000 Heating at 80 C 21000 Ultrasonication 17000 Example 4 5 mg of adriamycin hydrochloride and 5 mg of PE0-PBLA
(A-12-20) were added to 5 ml of 0.1 M Tris buffer, pH 9.1. Then, adriamycin was made miscible into micelles by stirring and ultrasonication.
Adriamycin is the compound of the following formula:
21040~
--- O OH
~COCH20H
CH O OH `o ~H3 , NH~
This compound itself does not dissolve in Tris buffer, pH 9.1, but can be completely dissolved according to the above procedure.
As shown in FIG. 4, adriamycin appeared in gel-exclusion volume in GPC where the sample was monitored at 485 nm at which adria-mycin shows characteristic absorption, and this indicates sufficient incorporation of adriamycin into micelles. In FIG. 4, elution volume is indicated as numerical values where 1.792, 3.292 and 9.300 mean micelles, a single polymer and unincorpo-rated adriamycin, respectively.
Example 5 4.4 ~11 triethylamine and 20 mg PE0-PBLA block copolymer (A-12-20) were added to a solution of 14 mg adriamycin hydrochlo-ride in 4 ml DMF, and the mixture was stirred for 10 min. and then dialyzed for 15 hours against distilled water. Dynamic light scattering indicated that the sample thus obtained formed polymeric micelles with a weight-average diameter of 55 nm. FIG.
5 shows a gel permeation chromatogram of the polymeric micelles monitored at 485 nm. Adriamycin was incorporated in the 21040~5 m~celles, as can be seen from its elution as micelles in gel exclusion volume (4.2-4.3 ml). FIG. 6 shows a gel permeation chromatogramofadriamycinincorporatedinmicellesafterallowed to stand for 5 hours in the presence of 50%(V/V) fetal bovine serum. In FIG. 6, the peak (4.25 ml) eluted in gel exclusion volume and not present in the serum itself was not lowered in the presence of serum (Fig. 7), which indicates that adriamycin can be stably maintained in micells even in the presence of serum.
Example 6 15 mg of indomethacin of formula CO -~ Cl ~N\~CH3 V~
CH30~ CH2COOH
as an anti-inflammatory drug was dissolved in 4 ml DMF, followed by addition of 20 mg of PE0-PBLA block copolymer (A-12-20). The mixture was stirred for 15 hours and dialyzed for 3 hours against 0.1 M phosphate buffer, pH 7.4, and then against water for 6 hours. The resulting sample was found to form polymric micelles with a weight-average diameter of 56 nm, as determined by dynamic light scattering. FIG. 8 shows a gel permeation chromatogram monitored at 312 nm at which indomethacin shows characteristic 21040~
absorption. The indomethacin was eluted as micelles in gel exclusion volume, indicating the incorporation of the indometha-cin into micelles. 0.76 mg of indomethacin was found to be incorporated in the micelles from its adsorption monitored at 312 nm in a solvent of DMF/distilled water (7: 3).
Claims (16)
1. A polymeric micelle type drug, which comprises an effective amount of a hydrophobic drug physically trapped in a drug carrier composed of a block copolymer represented by formula I or II:
R1(OCH2CH2)mR2COCHNH)nR4 I
¦
R1(OCH2CH2)mR2(NHCHCO)nR4 II
¦
[wherein:
R1 stands for H or an alkyl group, R2 stands for NH, CO, R6(CH2)qR7 (in which R6 represents OCO, OCONH, NHCO, NHCOO, NHCONH, CONH or COO, R7 represents NH or CO, and q represents 1-6), R3 stands for H, an alkyl group, (CH2)pC6H5, (CH2)pCOOR5 or CH2CONHR5 (in which p represents 1 or 2, R5 represents a C1-20 alkyl group, a benzyl-substituted C1-20 alkyl group or a benzyl group), R4 stands for H, OH or an alkyl group carrying CO, NH or O in the terminal, m stands for 4-2500, and n stands for 2-300].
R1(OCH2CH2)mR2COCHNH)nR4 I
¦
R1(OCH2CH2)mR2(NHCHCO)nR4 II
¦
[wherein:
R1 stands for H or an alkyl group, R2 stands for NH, CO, R6(CH2)qR7 (in which R6 represents OCO, OCONH, NHCO, NHCOO, NHCONH, CONH or COO, R7 represents NH or CO, and q represents 1-6), R3 stands for H, an alkyl group, (CH2)pC6H5, (CH2)pCOOR5 or CH2CONHR5 (in which p represents 1 or 2, R5 represents a C1-20 alkyl group, a benzyl-substituted C1-20 alkyl group or a benzyl group), R4 stands for H, OH or an alkyl group carrying CO, NH or O in the terminal, m stands for 4-2500, and n stands for 2-300].
2. The drug according to claim 1, in which the block copolymer is a compound represented by formula III:
III
(wherein m stands for 4-2500 and n stands for 2-300).
III
(wherein m stands for 4-2500 and n stands for 2-300).
3. The drug according to claim 1, in which the hydrophobic drug is adriamycin or indomethacin.
4. The drug according to claim 2, in which the hydrophobic drug is adriamycin.
5. The drug according to claim 2, in which the hydrophobic drug is indomethacin.
6. A method for producing the polymeric micelle type drug as defined in any one of claims 1 to 5, which comprises heating, ultrasonication or organic solvent treatment of the hydrophobic drug and the drug carrier to physically trap the hydrophobic drug in polymeric micelles composed of the drug carrier.
7. A polymeric micelle type drug, which comprises, in water, an effective amount of a hydrophobic drug physically trapped in a hydrophobic inner core of a micelle having a hydrophilic outer shell and the hydrophobic inner core, wherein the micelle is made of a drug carrier composed essentially of a block copolymer having hydrophilic and hydrophobic segments and being represented by the formulas I
[wherein:
R1 stands for H or an alkyl group;
R2 stands for NH, CO, R6(CH2)qR7 (in which R6 represents OCO, OCONH, NHCO, NHCOO, NHCONH, CONH or COO, R7 represents NH or CO and q represents 1-6);
R3 stands for an alkyl, CH2C6H5, (CH2)pCOOR5 or (CH2)pCONHR5 (in which p represents 1 or 2 and R5 represents a C1-20 alkyl group, a benzyl-substituted C1-20 alkyl group or a benzyl group);
R4 stands for H;
m stands for 4-2500; and n stands for 2-300].
[wherein:
R1 stands for H or an alkyl group;
R2 stands for NH, CO, R6(CH2)qR7 (in which R6 represents OCO, OCONH, NHCO, NHCOO, NHCONH, CONH or COO, R7 represents NH or CO and q represents 1-6);
R3 stands for an alkyl, CH2C6H5, (CH2)pCOOR5 or (CH2)pCONHR5 (in which p represents 1 or 2 and R5 represents a C1-20 alkyl group, a benzyl-substituted C1-20 alkyl group or a benzyl group);
R4 stands for H;
m stands for 4-2500; and n stands for 2-300].
8. The drug according to claim 7, wherein R2 in the formula I is NH.
9. The drug according to claim 8, wherein the hydrophilic segment is derivable from an alkyl ether derivative of polyethylene oxide and the hydrophobic segment is derivable from poly(.beta.-benzyl L-aspartate), poly(.gamma.-benzyl L-glutamate), poly(L-leucine), poly(L-valine) or poly(L-phenylalanine).
10. A polymeric micelle type drug, which comprises, in water, an effective amount of a hydrophobic drug physically trapped in a hydrophobic inner core of a micelle having a hydrophilic outer shell and the hydrophobic inner core, wherein the micelle is made of a drug carrier composed essentially of a block copolymer having hydrophilic and hydrophobic segments and being represented by the formula:
III
(wherein m stands for such a number that the portion CH3?OCH2CH2?mNH has a molecular weight of from about 200 to about 250,000, and n stands for such a number that the portion has a molecular weight of from 205 to about 62,000).
III
(wherein m stands for such a number that the portion CH3?OCH2CH2?mNH has a molecular weight of from about 200 to about 250,000, and n stands for such a number that the portion has a molecular weight of from 205 to about 62,000).
11. A method for producing the polymeric micelle type drug as defined in any one of claims 7-10, which comprises:
(1) heating at 30-100°C a mixture of the hydro-phobic drug and an aqueous micelle solution of the drug carrier, until the hydrophobic drug is incorporated into the micelles, (2) subjecting a mixture of the hydrophobic drug and an aqueous micelle solution of the drug carrier to ultrasonification until the hydrophobic drug is incorporated into the micelles, or (3) mixing an organic solvent solution of the hydrophobic drug and an aqueous micelle solution of the drug carrier to form a solution, and dialyzing the resulting solution against water.
(1) heating at 30-100°C a mixture of the hydro-phobic drug and an aqueous micelle solution of the drug carrier, until the hydrophobic drug is incorporated into the micelles, (2) subjecting a mixture of the hydrophobic drug and an aqueous micelle solution of the drug carrier to ultrasonification until the hydrophobic drug is incorporated into the micelles, or (3) mixing an organic solvent solution of the hydrophobic drug and an aqueous micelle solution of the drug carrier to form a solution, and dialyzing the resulting solution against water.
12. The method according to claim 11, wherein the method (3) is adopted; DMF is used as the organic solvent;
and the dialysis is conducted to cut off at a molecular weight of about 1,000.
and the dialysis is conducted to cut off at a molecular weight of about 1,000.
13. The method according to claim 11, wherein the method (2) is adopted.
14. A polymeric micelle type drug, which comprises an effective amount of a hydrophobic drug physically trapped in a drug carrier of a block copolymer comprising a hydrophilic segment selected from the group consisting of polyethylene oxide or its alkyl ether derivative, polymalic acid, polyasapartic acid, polyglutamic acid, polylysine, polysaccharide, polyacrylamide, polyacrylic acid, polymethacrylamide, polymethacrylic acid, polyvinylpyrrolidone, polyvinyl alcohol, polymethacrylate, polyacrylate, polyamino acid and derivatives thereof and a hydrophobic segment selected from the group consisting of poly(.beta.-benzyl L-aspartate), poly(.gamma.-benzyl L-glutamate), poly(.beta.-substituted aspartate), poly(.gamma.-substituted glutamate), poly(L-leucine), poly(L-valine), poly(L-phenylalanine), hydrophobic polyamino acid, polystyrene, polymethacrylate, polyacrylate, polymethacrylate amide, polyacrylate amide, polyamide, polyester, polyalkylene oxide (excluding polyethylene oxide) and hydrophobic polyolefin.
15. A polymeric micelle type drug according to claim 14, wherein the hydrophilic segment is polyethylene oxide.
16. A polymeric micelle type drug according to claim 14 or 15, wherein the hydrophobic segment is poly(.beta.-benzyl L-aspartate).
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JP5192586A JP2777530B2 (en) | 1992-08-14 | 1993-08-03 | Physical adsorption type polymer micelle drug |
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EP (1) | EP0583955B1 (en) |
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-
1993
- 1993-03-24 KR KR2019930004566U patent/KR940003548U/en not_active Application Discontinuation
- 1993-08-03 JP JP5192586A patent/JP2777530B2/en not_active Expired - Lifetime
- 1993-08-10 AU AU44523/93A patent/AU668967B2/en not_active Expired
- 1993-08-11 US US08/105,535 patent/US5449513A/en not_active Expired - Lifetime
- 1993-08-13 CA CA002104045A patent/CA2104045C/en not_active Expired - Lifetime
- 1993-08-13 ES ES93306397T patent/ES2141135T3/en not_active Expired - Lifetime
- 1993-08-13 EP EP93306397A patent/EP0583955B1/en not_active Expired - Lifetime
- 1993-08-13 DE DE69327490T patent/DE69327490T2/en not_active Expired - Lifetime
- 1993-08-14 KR KR1019930015734A patent/KR960009407B1/en not_active IP Right Cessation
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1995
- 1995-06-05 US US08/465,499 patent/US5510103A/en not_active Expired - Lifetime
Cited By (2)
Publication number | Priority date | Publication date | Assignee | Title |
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CN109642024A (en) * | 2016-08-02 | 2019-04-16 | 日本化药株式会社 | Active targeting type polymeric derivative, the composition comprising the polymeric derivative and their purposes |
US10973762B2 (en) | 2016-08-02 | 2021-04-13 | Nippon Kayaku Kabushiki Kaisha | Active-targeting-type polymer derivative, composition containing said polymer derivative, and uses of said polymer derivative and said composition |
Also Published As
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KR940003548U (en) | 1994-02-21 |
EP0583955A2 (en) | 1994-02-23 |
EP0583955B1 (en) | 2000-01-05 |
ES2141135T3 (en) | 2000-03-16 |
CA2104045A1 (en) | 1994-02-15 |
EP0583955A3 (en) | 1996-06-12 |
AU4452393A (en) | 1994-03-10 |
JPH06107565A (en) | 1994-04-19 |
AU668967B2 (en) | 1996-05-23 |
DE69327490T2 (en) | 2008-10-09 |
US5449513A (en) | 1995-09-12 |
KR940003548A (en) | 1994-03-12 |
KR960009407B1 (en) | 1996-07-19 |
US5510103A (en) | 1996-04-23 |
DE69327490D1 (en) | 2000-02-10 |
JP2777530B2 (en) | 1998-07-16 |
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