VACIK JIRI (CZ)
HOSEK PAVEL (CZ)
LABSKY JIRI (CZ)
VACIK JIRI (CZ)
HOSEK PAVEL (CZ)
| US4987210A | 1991-01-22 | |||
| EP0591024A2 | 1994-04-06 | |||
| DE19630977A1 | 1998-02-05 |
| 1. | l. ore their reactive derivatives, R6 is alkyl C1 C4, individually or in combination H, OH or oxxgen radical obtained by additional oxidation and W is selected from the group consisting of: O, OCH2,NH,NHCH2, where Rl to R4 is hydroxyalkyl, aminoalkyl, carboxyalkyl, CH (X) a CH (X) CHZ where X:COOH (halogenide, activated ester, mixed anhydride, azide),NCO, where n is 210, m is I10 ; derivatives of sterically hindered cyclic amines of the general formula (O) where R, to Ru are: alkyl CC_. (CH) n and n = 3 to 5, hydroxyalkyl, aminoalkyl, carboxyalkyl, in combinam. on and any representation, R6 is alkyl Cl to C4, H, OH or oxygen radical in any representation and W is represented by following groups:O, OCH2,NH,NHCH2,CH (X).CH (X) CH2, where X = and RI, R2 are alkyl C1 C10 ; polymers, copolymers, natural compound comprising free reactive groupsOH, NH2,COOH,CHO, oxirane, selected from the group poly (vinyl alcool), cellulose, (2hydroxyethyl) cellulose, (carboxymethyl) celullose, agar derivatives, polymers obtained by condensation, using dihydroxyalkane derivatives, oligomers and polymers of ethylene glycol or propylene glycol, natural or synthetic polymers, comprising free carboxyl groups, amino groups or aldehyde groups, prepared by additional functionalization of polymers or natural compound by polymeranalogous rection with a suitable sterically hindered amine selected from the group comprising: 4X1R62,2,6,6tetramethylpiperidine where X isNH2, iOH,halogen,NCO,COOH (halogenide, activated ester, mixed anhydride, azide),CH2Br and R6 is alkyl ClC4, individually or in combination H, OH or oxygen radical obtained by additional oxidation; 4 [ (nXalkyl) aminolIR62,2,6,6tetramethylpiperidine of the general formula mherse n = 1 to 10, X is halogen, OH, NH2, COOH, (halogenide, mixed anhydride, activated ester. azide). R6 is alkyl C1 C4, individually or in combination H, OH or oxygen radical obtained by additional oxidation: (1R62,2, 6,6tetramethylpiperidin4yl) (nl)Xalkanoate of a general formula: xhere n = 1 to 10, X is OH, NCO, COOH (halogenide, activated ester, mixed anhydride, azide).NCO, R is alkyl C1 C4, individually or in combination H, OH or oxygen radical obtained by additional oxidation: 4(nXalkyl)1R62, 2.6,6tetramethylpiperidine of the general formula: herse n = 110. X isNH..halogen,OH,NCO,COOH (halogenide, activated ester, rnixed anhydride. azide), R6 is alkyl C1 C4, individually or in combination H, OH or oxygen radical obtained by additional oxidation; «X1R62,2,5. 5tetramethylpyrrolidine of the general formula: shere X isNH2OH,NCO.COOH, (halogenide, activated ester, mixed anhydride, azide),CH Br, Ró is alkyl C,C4, individually or in combination H, OH or oxyoen radical obtained bvadditional oxidation : ofthegeneralformula:(1R62,2,5,5tetramethylpyrrolidin3yl)(n+1)Xalkanoate where n is 1 to 10, X isNH2OH,NCO,COOH (halogenide, activated ester, mixed anhydride, azide), R6 is alkyl ClC4, indiidually or in combination H, OH or oxygen radical obtained by additional oxidation; ', 2, 5,5tetramethyl2,5dihydropyrrole3carboxylic acid or acid derivative where A is COOH, (chloride, mixed anhydride, activated ester, azide), glycidyl ester, R is alkyl CIC4, individually or in combination H, OH or oxygen radical obtained by additional oxidation; 2. A preparation according to claim 1 comprising soluble polymers or copolymers of aliphatic amines prepared by radical polymerization using light, heat or LJV initiators in an amount of 0.01 to 10 by weight % based on the polymerization mixture, from monomers selected from the group consisting of: 3[NR6N(2methacryloylamino1,1dimethylethyl)amino]3methylbutanoicacid where R6 is alh1 ClC4, H, OH or oxygen radical obtained by additional oxidation; 3. A preparation according to claim 1 comprising soluble polymers or copolymers prepared by radical polymerization using light, heat or IJV initiators in an amount of 0.01 to 10 % by weight based on the polymerization mixture, from monomers comprising monomers of cyclic stericallyhindered amines selected from the group consistingof: (1R62,2,6,6tetramethylpiperidin4yl)acrylate,(1R62,2,6,6tetramethylpiperidin4 yl)methacrylate where R6 is alkyl C,C4, individually or in combination H, OH or oxygen radical obtained by additional oxidation; 1R62,2,6,6tetramethylpiperidine4yl(n+1)(acryloylamino)alkanoate ofthe(1R62,2,6,6tetramethylpiperidine4yl)(n+1)(methacryloylamino)alkanoate general formula R6 is alkyl C,C4, individually or in combination H, OH or oxygen radical obtained by additional oxidation; (2acryloyloxyethyl) 1R62,2,6,6tetramethylpiperidine4carboxylate (2methacryloyloxyethyl) 1R62, 2,6,6tetramethylpiperidine4carboxylate where R6 is alkyl ClC4, individually or in combination H, OH or oxygen radical obtained by additional oxidation; N (2,2,6,6tetramethylpiperidin4yl)acrylamide N(2, 2,6,6tetramethylpiperidin4yl) metliacrylamide 4acryloylaminolR62,2,6,6tetramethylpiperidine 4methacryloylamino1R62,2,6,6tetramethylpiperidine where R6 is alkyl C,C4, individually or in combination H, OH or oxygen radical obtained by additional oxidation N{m[(1R62,2,6,6tetramethylpiperidin4yl)carbamoyl]alkyl}acrylamide N {m[(1R62, 2,6,6tetramethylpiperidin4yl) carbamoylJalkyl} methacrylamide of the general formula: wliere m is 1 to 10, R6 is alkyl C1 C4, individually or in combination H, OH or oxygen radical obtained by additional oxidation; N(7R67azadispiro [5.1.5.3] hexadecan15yl) acrylamide N (7Rb7azadispiro [5.1.5.3] hexadecan15yl)methacrylamide R6 is alkyl C1C4, individually or in combination H, OH or oxygen radical.obtained by additional oxidation; N (lR62,2,5,5tetramethylpyrrolidin3yl)acrylamide N(1R62, 2,5,5tetramethylpyrrolidin3yl) methacrylamide where R6 is alkyl Cl to C4, individually or in combination H, OH or oxygen radical obtained by additional oxidation; N{n[(IR62,2,5,5tetramethylpyrrolidin3yl) carbamoyl] alkyl} acrylamide N {n[(lR62,2,5,5tetramethylpyrrolidin3yl) carbamoyl] alkyl} methacrylamide where n is 1 to 10, R6 is alkyl ClC4, individually or in combination H, OH or oxygen radical obtained by additional oxidation; 1R62,2,5,5tetramethylpyrrolidin3ylacrylate, 1R62,2,5,5tetramethylpyrrolidin3ylmethacrylate where R6 is alkyl ClC4, individually or in combination H, OH or oxygen radical obtained by additional oxidation; 1R62,2,5,5tetramethylpyrrolidin3yl (n+1) (acryloylamino) alkanoate ofthe1R62,2,5,5tetramethylpyrrolidin3yl(n+1)(methcryloylamino)alkanoate generalformula where n is l to 10. R6 is alkyl C1 C4, individually or in combination H, OH or oxygen radical obtained by additional oxidation; 2acryloyloxyethyl1R62,2,5,5tetramethyl2,5dihydropyrrole3carboxylate, 2methacryloyloxyethylIR62, 2, 5,5tetramethyl2,5dihydropyrrole3carboxylate where R6 is alkyl C I to C4, individually or in combination H, OH or oxygen radical obtained by additional oxidation; (1R64carboxy2, 2,6,6tetramethylpiperidin4yl) acrylate, (1R64carboxy2, 2,6,6tetramethylpiperidin4yl) methacrylate where R6 is alkyl C,C4, individually or in combination H, OH or oxygen radical obtained by additional oxidation, 1(2, 2,6,6tetramethylpiperidin4yl)2,5dihydropyrrole2,5dione of the general formula: where R6 is alkyl ClC4, individually or in combination H, OH or oxygen radical obtained by additional oxidation; (1R42,2,6, 6tetramethylpiperidin4yl)acrylate (1R62,2,6,6tetramethylpiperidin4yl)methacrylate wliere R6 is alkyl C1C4, individually or in combination H, OH or oxygen radical obtained by additional oxidation; 4R61acryloyl3, 3,5,5tetramethylpiperazine 4R61methacryloyl3, 3,5,5tetramethylpiperazine of the general formula where R6 is alkyl C1 C4, individually or in combination H, OH or oxygen radical obtained by additional oxidation; N {n [ (7R67azadispiro [5.1.5.3] hexadecan15yl) carbamoyl] alkyl} acrylamide N {n [ (7R67azadispiro [5.1.5.3] hexadecan15yl) carbamoyl]alkyl} methacrylamide offormula:general where n is I to 10 and R6 is alkyl C1 C4, individually or in combination H, OH or oxygen radical obtained by additional oxidation ; N{(n+1)oxon[(7R67,15diazadispiro[5.1.5.3]hexadecan15yl)alkyl]}acrylamide Nt (n+l)oxon [ (7R67, 15diazadispiro [5. 1.5. 3] hexadecan15yl) alkyl]} methacryl amide of the general formula: where n is l to 10, R6 is alkyl C1 C4, H, OH, oxygen radical in any representation, 2methacryloyloxyethyl propanoate where R6 is alkyl C IC4, individually or in combination, H, OH or oxygen radical obtained by additional oxidation. |
| 2. | 4 A preparation according to claims l to 3, wherein the amino groups present in the polxmer are partly or totally neutralized by an acid selected from the group hydrogen halogenide, acetic acid, propionic acid, sulfuric acid, citric acid, 4methylbenzene sulfonic acid and cinnamic acid. |
| 3. | A preparation according to claims 1 to 4 prepared from a polymerization mixture comprising vinyl monomers selected from the group consisting of acrylic acid and methacrylic acid, alkyl acrylates and methacrylates, hydroxyalkyl acrylates and methacrylates, (alkyloxy) alkyl acrylates and methacrylates, (acyloxyalkyl) acrylates and methacrylates, acrylamides and methacrylamides, substituted Nalkylacrylamides and Nalkylmethacrylamides, N (hydroxyalkyl) acrylamides and N (hydroxyalkyl) methacrylamides, lvinyl2pyrrolidone, diacetonacrylamide [N (1,1 dimethyl3oxobutyl) acrylamide]. |
| 4. | A preparation according to claims l to 5, prepared from a polymerization mixture comprising 0.01 to 40 % of crosslinking agent selected from the group consisting of: 1, 1'divinyl3, 3' (ethane1, 1diyl) di (2pyrrolidone) of the formula: ethylene diacrylate, ethylene dimethacrylate of the formula: poly (ethylene glycol) diacrylate, poly (ethylene glycol) dimethacrylate of the general formula where n is 2 to 20. |
| 5. | A preparation according to claim 1 prepared from a polymerization mixture comprising a polymerizable tertiary amine or polymerizable quaternary ammonium salt in a concentration 1.0 x106 to 10 % by weight based on the whole mixture selected from the group consisting of: 1alkyl4 (or 2or 3) vinylpyridinium halogenide of the formula: N[n(acryloyloxy)[n(acryloyloxy) alkyl)]N, NdialkylNmethylammonium halogenide N[n(methacryloyloxy)[n(methacryloyloxy) alkyl)]N, NdialkylNmethylammonium halogenide of the general formula where n is 2 to 10, N[n(acryloylamino)alkyl)]N,NdialkylNmethylammoniumhalogenide N [n (methacryloylamino) alkyl))N, N dialkylNmethylammonium halogenide of the general formula: where n is 2 to 10, a polymerizable tertiary amine, where the quaternary salt is obtained by additional quaternization 4 (or 2or3)vinylpyridine of the formula: N[n(acryloylamino)alkyl]dialkylamine N[n(methacryloylamino)[n(methacryloylamino) alkyl] dialkylamine of the general formula: where n is'to 10. n(N,Ndialkylamino)alkylacrylate n(N,Ndialkylamino)alkyl methacrylate of the general formula: where n to10,2 R2, alkylC1C4,is tosyl,acetate,citrate,sulfate,cinnamate,toluene4sulfonate.X#:halogen, 8. A preparation according to claim 1 comprising soluble polymers prepared by condensation of difunctional sterically hindered amines selected from the group consisting of: 2, 2,2',2'tetramethyl2,2'(R6imino) di (ethanamine) (where X is NH2) or where X is OH, COOH (chloride, mixed anhydride, activated ester, azide), NCO, R6 is alkyl C,C4. individuallv or in combination H, OH or oxygen radical obtained by additional oxidation; 1,1'(R6imino) di (cyclohexanecarboxylic acid) (where X is COOH) of the general formula: where X is COOH, (halogenide, mixed anhydride, activated ester, azide), NCO, NH2, OH. CH26HI2, R6 is alkyl C,C4, individually or in combination H, OH or oxygen radical obtained by additional oxidation. 9. A preparation according to claim 1 prepared from a polycondensation mixture comprising difunctional, cyclic, sterically hindered amines selected from the group consisting of: 2(1R62, 2,6,6tetramethylpiperidin4yl) succinic acid where X isCOOH. X isCH20H, CH2NH2,COOH (chloride, mixed anhydride, activated ester, azide),CH2NH2,NCO, R6 is alkyl ClC4, individually or in combination H, OH or oxygen radical obtained by additional oxidation; 4 [ (nXalkyl) amino]lR62,2,6,6tetramethylpiperidine of the general formula: where X isNH2,OH,COOH, n is equal to 210, R6 is alkyl ClC4, individually or in combination H, OH or oxygen radical obtained by additional oxidation; N, Nbis (1R62,2,6,6tetramethylpiperidin4yl) alkane1, mdiamine of the general formula: where m is 2 to 10, N, N'bis(1R62, 2,5,5tetramethylpyrrolidin4yl) alkanel, mdiamine of the general formula: where m is = to 10. P,6 is alkyl C1C. indiidually orin combination H, OH or oxygen radical obtained by additional oxidation: 4aminolR2,2, 5,5tetramethylpyrrolidine3carboxylic acid of the general formula: R6 is alkyl C _C4, individually or in combination H, OH or oxygen radical obtained by additional oxidation; 3, 3'(1R62,2, 6, 6tetramethylpiperidine4,4diyl) di (propanoic acid) (X isCOOH) where X isNH2, OH, COOH (chloride, mixed anhydride, activated ester, azide), NCO, R6 is alkyl C 1C4, individually or in combination H, OH or oxygen radical obtained by additional oxidation; thegeneralformula:3[(nXalkyl)amino]1R62,2,5,5tetramethylpyrrolidineof X is NH2, OH, COOH (chloride. mixed anhydride, activated ester, azide), n is 2 to 10, R6 is alkyl C1 C4, individually or in combination H, OH or oxygen radical obtained by additional oxidation; αhydro#[(1R62,2 6,6teTramethylpiperidin4yl) amino] poly (oxyethylene) of the gen,ral fomiula: where n is 1 to 100. R6 is alkyl C1 C4, individually or in combination H, OH or oxyaen radical obtained by additional oxidation: <BR> <BR> α{2[(1R62,2,6,6tetramethylpiperidin4yl)amino]#[(1R62,2,6,6tetramethyl piperidin4yl)amino]poly(oxyethylene) where n is l to 10. R6 is alkyl CsC4, individually or in combination H, OH or oxygen radical obtained by additional oxidation. |
| 6. | 10 A preparation according to claim 1 prepared by polycondensation in the presence of diftmetional monomers selected together from the group A and B of compound of the followine general formulas: where Z is KH,CH2, nits l to 100. m is 2 to 12. |
| 7. | _A preraration according to claims 9 and 10 prepared from a polycondensation mixture comprising in an amont of 0.01 to 15% monofunctional cyclic sterically hindere3 amine selected from the group consisting of: thegeneralformula:4X1R62,2,6,6tetramethylpiperidineof XZhere X isNH.OH.NCO,COOH (chloride, activated ester, mixed anhydride, individually or in combination H, OH or oxygen radical obtained by additional oxidation: α(2Xethyl)#(1R62, 2,6,6tetramethylpiperidin4yloxy) poly (oxyethylene) of the general formula where n is = 1 to 100. X is NH2 NCO, COOH (chloride, activated ester, mixed anhydride, azide), R6 is aLhl CzC4, individually or in combination H, OH or oxygen radical obtained by additional oxidation; (nXalkyl)1R62, 2,5,5tetramethylpyrrolidine3carboxylate where n = 2 to 10, X is OH, NH2, NCO, COOH (halogenide, azide, mixed anhydride, activated ester), R6 is alkyl C:C4, individually or in combination H, OH or oxygen radical obtained by additional oxidation; 4(nXalkyl)2,2, 6,6tetramethyl1R6piperidine ofthe general formula where n = 110. X is NH2*OH.NCO,COOH (halogenide, activated ester, mixed anhydride, azide), R5 is alkyl C@ C4, individually or in combination H, OH or oxygen radical obtained by additional oxidation N(1R@2,2,6,6tetramethylpiperidin4yl)[(n+1)Xalkaneamide] xrhere n = 110, X isNH2,OH,NCO,COOH (halogenide, activated ester, mixed anhydride, azide), R@ is alkyl C1 C4, individually or in combination H, OH or oxyszen radical obtained by additional oxidation ofthegeneralformula:1R62,2,6,6tetramethylpiperidin4yl)(n1)Xalkanoate where n is 1 = 10, X isNH2,OH,NCO,COOH (halogenide, activated ester, mixed anhydride, azide, R6 is alkyl Cl to C4, individually or in combination H, OH or oxygen radical obtained bv additional oxidation; 3X1R62,2,5,5tetramethylpyrrolidine whe e X isNH.OH.NCO,COOH (halogenide, activated ester, mixed anhydride, azide), R6 is alkyl C1 C4, individually or in combination H, OH or oxygen radical obtained by additional oxidation. |
| 8. | A preparation according to claims 8 11 prepared from the polymerization mixture comprising 0.1 tu =0 %, based on the polymerization mixture of a crosslinking agent selectedselectedfrom the of:consisting 2,2', Is (hydroxymethyl) alkanol where n is @ to 10, 2,2*ó 6tetrakis (hydroxymethyl) cyklohexanol 2,2',6,6'tetrakis(hydroxymethyl)4,4'methylenedicyclohexanone pentane1,3,5triol 2,2iminodi (ethanamine) @,2bis@hydroxymethyl)1,3propandiol 13. A preparation according to claim 8 to 11 prepared from a polycondensation mixture ammoniumsaltsorsubsequentlyquaternizedprecursorscomprisingquaternary capable of condensation selected Som the group consisting of: thegeneralformula:n(N,Ndialkylamino)alkanolof Xrhere n = 2 to 10, n(N,Ndialkylamino)alkylamine of the general formula: =2to10,wheren n(hydroxyalkyl)N,NdialkylNmethylammonium halogenide of the general formula: where n = 2 to 10, naminoalkylN,NdialkylNmethylammonium halogenide of the general formula: =2to10.wheren 14. A preparation according to claims 1 to 5,7 to 13 consisting of composite systems, obtained by their mixing with other polymers selected from the group consisting of poly (Nvinylpyrrolidone), poly (vinyl alcool), poly (2hydroxyethyl methacrylate), poly (sodium acrylate), poly (sodium methacrylate), agar, gelatin. |
| 9. | 15 A preparation according to claim 14 wherein a soluble composite system is dissolve in a suitable monomer selected from the group consisting of Nvinylpyrrolidone, 2hydroxyethyl methacrylate, sodium acrylate and subsequently polymerized to a soluble or insoluble composite material. |
| 10. | 16 A preparation according to claim 14 wherein a soluble composite system is present in a mixture comprising polymers susceptible to polycondensation selected from the group consisting of poly (ethylene glycol), poly (propylene glycol), a, coalkanediols, a, a)alkanediamines, alkanedioic acids (halogenide, activated esters, diazides), a, co alkanediyl isocyanates. |
| 11. | 17 A preparation according to claim 14 to 16, wherein composite systems comprise 0.1 to 15 % by weight of derivatives of sterically hindered cyclic amines of the general formula: where R, to R4 are alkyl C,C4, (CH2) n and n is equal to 3,4,5, hydroxyalkyl, aminoalkyl, carboxyalkyl, in various combination and various representation, R6 is alkyl ClC4, individually or in combination H, OH or oxygen radical obtained by additional oxidation; and W represents the following groups:O, OCH2,CH (X), CH(X)CH2,OCH(X),Xis:OH,NH2,COOH,NHR1,NH,NHCH2, NRIR2, NHCOR, COOR where RX, R2iS alkyl ClC4 18. A preparation according to claim 1 comprising derivatives of sterically hindered cyclic amines selected from the group consisting of: 4X1R62,2,6,6tetramethylpiperidine where X isOH,COOH, acyloxy, acylamino group and R6 is alkyl C IC4, individually or in combination H, OH or oxygen radical obtained by additional oxidation; α(1R62,2,6,6tetramethylpiperidine4carbonyl)#(1R62,2,6,6tetramethyl piperidine4carbonyloxy) poly (oxyethylene) oc(1R62,2,6, 6tetramethylpiperidine4carbonyl)#(1R62, 2,6,6tetramethyl piperidine4carbonyloxy) poly [oxy (1methylethylene)] R is H or CH3, n is 1 to 100, R6 is alkyl ClC4, individually or in combination H, OH or oxygen radical obtained by additional oxidation; a(1R62,2,5, 5tetramethylpyrrolidine3carbonyl)#(1R62, 2,5,5tetramethyl pyrrolidine3carbonyloxy) poly [oxy (1methylethylene)] where n is 1 to 100 and R isCH3 R is H or CH3, n is 1 to 100. α(1R62, 2,5,5tetramethyl2,5dihydropyrrole3carbonyl)@(1R62,2,5,5 tetramethyl2,5dihydropyrrole3carbonyloxy) poly (oxyethylene) α(1R62, 2,5,5tetramethyl2,5dihydropyrrole3carbonyl) (o(lR62, 2,5,5 tetramethyl2,5dihydropyrrole3carbonyloxy) poly [oxy (1methylethylene)] R is H or CH3, n is 1 to 100. |
| 12. | 1R62,2,5,5tetramethylpyrrolidine3carboxylic acid where X isCOOH,OH,NH2, acyloxy, acylamino group, R6 is alkyl ClC4, individually orin combination H, OH or oxgen radical obtained by additional oxidation; 1R62,2,5,5tetramethyl2,5dihydropyrrole3carboxylicacid where Y isCOOH, R6 is alkyl ClC4, individually or in combination H, OH or oxygen radical obtained by additional oxidation; N, N'bis (1R62,2,5,5tetramethylpyrrolidin3yl) alkanediamide where n = 1 to 10, R6 is alkyl ClC4, individually or in combination H, OH or oxygen radical obtained by additional oxidation, N, N'(1, nalkanediyl) di (lR62,2,5,5tetramethyl2,5dihydropyrrole3carboxamide where n = 2 to 10. |
| 13. | A preparation according to claim 18 present in an amount of 0.1 to 15 % by weight in composite systems, obtained by their mixing with other polymers selected from the group consisting of poly (1vinyl2pyrrolidone), poly (vinyl alcool), poly (2 hydroxyethyl methacrylate), poly (alkyl acrylate), poly (alkyl methacrylate), agar, gelatin. |
| 14. | A preparation according to claim 18 present in an amount of 0.1 to 15 % by weight in composite systems dissolve in a suitable monomer selected from the group consisting of 1vinyl2pyrrolidone, 2hydroxyethyl methacrylate, 2acetoxyethyl methacrylate, acrylic acid, methacrylic acid, 2 (2hydroxyethoxy) ethyl methacrylate and subsequently polymerized to a soluble or insoluble composite material. |
| 15. | A preparation according to claim 17 present in an amount of 0.1 to 15% by weight in a composite mixture comprising polymers susceptible to polycondensation selected from the group consisting of poly (ethylene glycol), poly (propylene glycol), alkanea, wdiols, alkanea, wdiamines, alkanedioyldihalogenides, diisocyanates. AMENDED CLAIMS [received by the International Bureau on 03 April 1999 (03.04.99); original claims 2,3 and 7 amended; remaining claims unchanged (4 pages)] where n is 1 to 10, X isNH2,OH,NCO,COOH (halogenide, activated ester, mixed anhydride, azide), R6 is alkyl C,C4, individually or in combination H, OH or oxygen radical obtained by additional oxidation; 2,2,5,5tetramethyl2,5dihydropyrrole3carboxylic acid or acid derivative where A isCOOH, (chloride, mixed anhydride, activated ester, azide), glycidyl ester, R6 is alkyl ClC4, individually or in combination H, OH or oxygen radical obtained by additional oxidation; 2. A preparation according to claim l comprising soluble polymers or copolymers of aliphatic amines prepared by radical polymerization using light, heat or UV initiators in an amount of 0.01 to 10 by weight % based on the polymerization mixture, from monomers selected from the group consisting of : 3 [NR6N(2acryloylaminol, 1dimethylethyl) amino]3methylbutanoic acid 3[NR6N(2methacryloylamino1,1dimethylethyl) amino]3methylbutanoic acid where R6 is alkyl ClC4, H, OH or oxygen radical obtained by additional oxidation. |
| 16. | 3 A preparation according to claim 1 comprising soluble polymers or copolymers prepared by radical polymerization using light, heat or UV initiators in an amount of 0.01 to 10 % by weight based on the polymerization mixture, from monomers comprising monomers of cyclic sterically hindered amines selected from the group consisting of : N(2,2,6,6tetramethylpiperidin4yl)methacrylamide 1R64acryloylamino2,2,6,6tetramethylpiperidine, 1R64methacryloylamino2,2,6,6tetramethylpiperidine isalkylC1C4,individuallyorincombinationH,OHoroxygenradicalwhereR6 additionaloxidation;obtainedby N{m[(1R62,2,6,6tetramethylpiperidin4yl)carbamoyl]alkyl}acrylamide N{m[(IR62,2,6,6tetramethylpiperidin4yl)carbamoyl]alkyl}methacrylamide of trie general formula: wherewherem is 10,R6isalkylC1C4,individuallyorincombinationH,OHorto oxygen radical obtnined by additionnl oxidation; N(7R67azadispiro[5.1.5.3]hexadecan15yl)acrylamide N(7R67azadispiro[5.1.5.3]hexadecan15yl)methacrylamide alkylC1C4,individuallyorincombinationH,OHoroxygenradical,obtainedR6is byadditional oxidation; 1R62, 2,5, 5tetramethylpyrrolidin3yl (n+1)(methacryloylamino)alkanoate of thc generalformula where n is l to 10. R6 is alkyi C,C4, individually or in combination EX, OH or oxygen radical obtained by additional oxidation ; 2acryloyloxyethyl lR62,2,5,5tetramethyl2,5dihydropyrrole3carboxylate, 2methacryloyloxyethyl 1R62,2,5,5tetramethyl2,5dihydropyrrole3carboxylate where R6 is alkyl C, to C4, individually or v combination H, OH or oxygen radical obtained by additional oxidation; 1R64acryloylox2, 2,6,6tetramethylpiperidine4carboxylate 1R64methacryloyloxy2,2,6,6tetramethylpiperidine4carboxylate where R6 is alkyl ClC4, individually or in combination H, OH or oxygen fadical obtained by additional oxidation, 1(2, 2,6,6tetramethylpiperidin4yl)2,5dihydropyrrole2,5dione of the general formula: halogen, tosyl, acetate, citrate, sulfate, cinnamate, toluene4 sulfonate, N[n(acryloyloxy)alkyl)]N,NdialkylNmethylammoniumhalogenide Nrn(methacryloylo, xyEalk,(methacryloylo, xyEalk, yl)]N, NdialkylNmethylammonium halogenide of the general formula halogen, tosyl, acetate, citrate, sulfate, cìnnamate, toluene4sulfonate, lvhere n is 2 to 10, Nrn(acryloylamino) alkyl) lN,(acryloylamino) alkyl) lN, NdialkylNmethylammonium halogenide N[n(methacryloylamino)alkyl)]N,NdialkylNmethylammoniumhalogenide of the general formula: halogen, tosyl, acetate, citrate, sulfate, cinnamate, toluene4sulfonate, where n is 2 to 10, a polymerizable tertiary amine, where the quaternary salt is obtained by additional quaternization 4(or 2or3)vinylpyridine(or 2or3)vinylpyridine of the formula: N [n (acryloylamino) alkyljdialkylamine N (n (methacryloylamino) alkylldialkylamine of the general formula:. |
Background Art Due to the effect of various types of radiation such as LTV, gamma, X-ray and similar radiation as well as hyperoxia, xenobiotic, upon injury or as a result of certain diseases, the living organisms, may suffer from surface lesion affecting the skin, fascia, and muscle in different depth. Upon any injury a massive proliferation of radicals occurs due to the oxygen reduction accompanied by generation of reactive oxygen compound.
The reason for the radical proliferation is a defect in coordination of redox enzymatic systems of the living tissue under injury as well as the activity of the leukocytes present.
The reactive oxygen compound, mostly of radical nature, have agressive impact on biological systems and produce often irreparable changes, for example in rection with lipids, proteins, or DNA and cause damage to physiological protective mechanisms preventing the biological systems from the adverse effect of reactive oxygen products.
Simultaneously, enzymatic systems are activated, which contributes to the generation of the reactive oxygen products.
The protective systems present physiologically in the living organisms are low- molecular weight compound such as vitamins C, E, glutathione or macromolecular compound such as enzymes, catalase, superoxide dismutase, glutathione, reductase, peroxidase or cyclooxygenases. In the event of a deep tissue damage the aforesaid compound align with the phagocyte activity of leukocytes are not able to control the proliferation of free radicals to the extent which could ensure a satisfactory healing effect.
If a wound is attacked by bacteria, the reactive oxygen radicals may cause damage to the tissue but, on the other hand, they are not enough to stop the bacteria
growth, which results in the degradation of the tissue macromolecules and in the accompanying penetration of leukocytes, which is the major reason for a pyogenic process. Subsequently, even if the production of bacterial flora is controlled, such radicals cause an excessive cytokine production, which promotes the growth of fibroblasts and, due to copious granulation, the epithelization is going down, which again results in a delayed healing process.
The conventional medical treatment mostly concentrates on the inflammation stage (using bacteria eliminating antibiotics, granulation medicaments, including prostaglandins) and is mostly insufficient in the epithelization stage, for example, a treatment of the wound may occur, however, granulations are poor or granulations are copious but the wound fails to come to epithelization.
Summary of Invention The object of the invention of a preparation for prevention and healing of inflammation affections is to eliminate, to a considerable extent, the above inconvenience. The preparation comprises 0.1 to 99.9 % by weight, derivatives of sterically hindered amines selected from the group consisting of : soluble polymers or copolymers prepared by radical polymerization in the presence of 0.01 to 10% by weight of initiators in polymerization mixture comprising individually or in combination an aliphatic amine monomer of the general formula (A): where RA to RF are: alkyl Cl-C4,- (CH2) n-and n = 3,4,5, polymerizable vinyl group in various combination and representation, R6 is alkyl Cl C4, individually or in any combination, H, OH or oxygen radical obtained by additional oxidation; soluble polymers or copolymers prepared by radical polymerization in the presence of 0.01 to 10% by weight of initiators, from monomers of cyclic sterically hindered amines of general formula (B) where Rl to R4 are: alkyl C,-C4,- (CH2),- and n = 3,4,5, R6 is alkyl Cl-C4, individually or in any combination, H, OH or oxygen radical obtained by additional oxidation and W is selected from the group including-CH (X)- a-CH (X) CH2-where X is: -N (X)- and N (X) CH2- where X is:
-O-,-OCH2-, and Rl to R4 is a radical having one polymerizable vinyl group; soluble polymers prepared by polycondensation of difunctional sterically hindered amines of the general formula (F) where RA to RF are: alkyl Cl to C4,- (CH2),- and n = 3,4,5, hydroxyalkyl, aminoalkyl, carboxyalkyl (halogenide, activated ester, azide), isocyanatoalkyl in various combination and representation, R6 is alkyl C,-C4, individually or in combination H, OH or oxygen radical obtained by additional oxidation; soluble polymers or copolymers prepared by polycondensation of difunctional cyclic sterically hindered amines of the general formula (G) where R1 to R4 are: alkyl C1 - C4, -(CH2)n- and n = 3,4,5, hydroxyalkyl, aminoalkyl, carboxyalkyl (halogenide, activated ester, azide), isocyanatoalkyl, R6 is alkyl Cl C4, individually or in combination H, OH or oxygen radical obtained by additional oxidation and W is selected from the group-O-,-OCH2-,-NH-,-NHCH2-where Rl-R4 is hydroxyalkyl, aminoalkyl, carboxyalkyl (halogenide, activated ester, azide), isocyanatoalkyl)-CH (X)-,-CH (X) CH2-, where X is:
1tonis 10, 2to10is where A, B are-OH,-NH2,-COOH; soluble copolymers prepared by polycondensation of difunctional cyclic, sterically hindered amines of the general formula (G) and monofunctional cyclic sterically hindered amines in an amount of 0.1 to 15 %. by weight, based on the total polymerization mixture of the general formula (H) where Rl to R4 are: alkyl C1 - C4, -(CH2)n and n = 4 or 5, hydroxyalkyl, aminoalkyl, carboxyalkyl, ore their reactive derivatives, R6 is alkyl Cl-C4, individually or in combination H, OH or oxygen radical obtained by additional oxidation and W is selected from the group consisting of :-O-, OCH2-,-NH-,-NHCH2-, where R, to R4 is hydroxyalkyl, aminoalkyl, carboxyalkyl, CH (X)- a CH (X) CH2- where X:-COOH (halogenide, activated ester, mixed anhydride, azide),-NCO, where n is 2-10, m is 1 - 10 ; derivatives of sterically hindered cyclic amines of general formula
where R, to R4 are: alkyl C,-C4,- (CH2) n and n = 3 to 5, hydroxyalkyl, aminoalkyl, carboxyalkyl, in combination and any representation R6 is alkyl Cl to C4, H, OH or oxygen radical in any representation and W is represented by following groups:-O-, -OCH2-,-NH-,-NHCH2-,-CH (X)-.-CH (X) CH2-, where X = and RI, R2 are alkyl C1 - C10 ; polymers, copolymers, natural compound comprising free reactive groups-OH,-NH2, -COOH,-CHO, oxiran, selected from the group consisting of poly (vinyl alcool), cellulose, (2-hydroxyethyl) cellulose, (carboxymethyl) celullose, agar derivatives, polymers obtained by condensation, using dihydroxyalkane derivatives, oligomers and polymers of ethylene glycol or propylene glycol, natural o synthetic polymers, comprising a free carboxyl group, amino group or aldehyde group, prepared by additional functionalization of polymers or natural compound by polymer-analogous rection with a suitable sterically hindered amine selected from the group comprising: 4-X-1-R6-2,2,6,6-tetramethyl-piperidine where X is-NH2, i-OH,-halogen,-NCO,-COOH (halogenide, activated ester, mixed anhydride, azide),-CH2Br and R6 is alkyl Cl-C4, individually or in combination, H, OH or oxygen radical obtained by additional oxidation; (n-X-alkyl)-l-R6-(2,2,6,6-tetramethyl-piperidin-4-yl) amine of the general formula
where n = 1 to 10, X is halogen,-OH,-NH2,-COOH, (halogenide, mixed anhydride, activated ester, azide), R6 is alkyl C,-C4, individually or in combination, H, OH or oxygen radical obtained by additional oxidation, 1-R6-(2, 2,6,6-tetramethylpiperidin-4-yl)- (n+1)-X-alkanoate of general formula
where n = 1-10, X is-OH,-NCO,-COOH (halogenide, activated ester, mixed anhydride, azide),-NCO, R6 is alkyl C,-C4, individually or in combination, H, OH or oxygen radical obtained by additional oxidation; 4-(n-X-alkyl)-l-R6-2,(n-X-alkyl)-l-R6-2, 2,6,6-tetramethylpiperidine of the general formula:
where n =1-101 X is-NH2,-halogen,-OH,-NCO,-COOH (halogenide, activated ester, mixed anhydride, azide), R6 is alkyl Cl-C4, individually or in combination, H, OH or oxygen radical obtained by additional oxidation; 3-X-1-R6-2,2,5,5-tetramethylpyrrolidine of general formula: where X is -NH2. -OH, -NCO, -COOH, (halogenide, activated ester, mixed anhydride, azide).-CH2Br. R6 is alkyl C : to C_. indiwidually or in combination, H, OH or oxygen radical obtained by additional oxidation; 1-R6-(2,2,5,5-tetramethyl-pyrrolidin-3-yl) (n~1)-X-alkanoate of the general formula:
where n is 1 to 10, X is -NH2, -OH, -NCO, -COOH (halogenide, activated ester, mixed anhydride, azide), R6 is alkyl C1 - C@, individually or in combination, H, OH or oxygen radical obtained by additional oxidalion; 1-R6-2.2, 5,5-tetramethvl-2, 5-dihydropyrrole-3-carboxylic acid where A is-COOH, (hloride. mixed anhydride, activated ester, azide), glycidyl ester, R6 is alkyl C1 - C4, individually or in combination, H, OH or oxygen radical obtained by additional oxidation.
Further developments and improvements of the invention are demonstrated by reference to various compound which are subject to dependent claims and the preparation and effets of which are demonstrated in the accompanying examples. The invention is based on a new finding that amines with sterically hindered amino groups are able to substantially liquidate reactive oxygen derivatives and thus to enable accelerated healing of damaoed tissues. The mechanism of their effect on the living organism has not been described, howe-er, the chemism of the elimination of the oxygen reactive radicals may be similar to that described for the polymeric systems. The presence of ans ouf the oxidation states of such amines (hydroxylamine or nitroxide) accelerates the healina of damaged tissues since, due to the recombination with free radicals or oxidation agents. such as hydrogen peroxide, organic peroxy radicals, hyperoxides, etc. formed in the living tissue, a considerably larger spectrum of compound for their liquidation is available.
The compound contain : d in W e preFaration according to the invention include soluble or crosslinked polymers, which are formed from polymerizable sterically hindered amines or copolymers, wherein. besides a sequence formed from a polymerizable amine, any suitable monomer may be incorporated, advantageously a hydrophilic one. The accessibility of the amino group is from the steric point of view substantially restricted. The stabile free radicals derived from that group of compound are not able to initiate a radical polwnerization. The sterically hindered amines may survive the polymerization in their original form or, i. e., as amine or, as the case may be, in a higher oxidation state i. e. as hydroxylamine or nitroxide.
This type of amines or their derivatives preferably react with oxygen and its reduced derivatives such as superoxide, hydroxyl radical, hydrogen peroxide, alkyl peroxides, alkyl hyperoxides, etc. and protect the tissue from destructive oxidation. The hydrophilic polymers are suitable for applications in medicine in the form of gels, foils, therapeutic contact lenses. powders, etc. In a proper configuration such as foam, sponge, etc. The aforesaid polymeric systems may simultaneously remove water from the injured tissues.
The same effect results in production of polymers prepared by condensation of di-or polyfunctional alcool, amines. aminoalcohol with reactive derivatives of di-and polyfunctional acid derivatives such > chlorides, activated esters, mixed anhydrides, or bifunctional isocyanates, upon formation of polyesters, polyamides, urethanes or their combination compound. In such polymers formed by condensation, it is of course assumed that they contain a built-in sterically hindered amine provided with suitable reactive groups. Such polymers prepared by condensation may be prepared, dependent on the polymerization condition. in a soluble or crosslinked form.
In connection with the new preparation, the antibacterial effect of quaternary ammonium salts may be used and in this case the therapeutic effect of the polymeric derivatives of the sterically hindered amines and their oxidation derivatives may be combine with the therapeutic effect of the polymeric derivatives of quaternary ammonium salts in order to achève substantially prolonge period, which may be necessary for the application of polzleric systems, without causing a contamination.
The enhanced antibacterial effect, for example with a denture prosthesis may be secured by the presence of bonded quaternary ammonium salts which may be prepared by copolymerization of the above specified polymerization mixtures with the polymerizable quaternar salts or precursors thereof and their subsequent quaternization
or by conden : ation ot substituted amines in such a manner that the quaternization may be carried out subsequently.
The method of preparation of copolymers consists in the polymerization of a polymerization mixture including some of the above described vinyl monomers or a combination thereof. a polymerizable sterically hindered amine or a mixture thereof or, as the case mav be a hydroxylamine derivatis-e and, if necessary, a crosslinking agent and initiator uoder tormation of a soluble or insoluble polymer powder or a required article forme in the polymerization mold such as foil, lens, etc. In preparation of hydrophilic gel articles, the process may be managed in such a way that in the first stage powdered hs-drophilic polymers-ith a sterically hindered amine and amino group in varioui oxidation state represented by amine, hydroxylamine, or nitroxide radical or varions types of derivatives of stericall hindered secondary amines in the form of powdered polvmers havin various oxidation state which may be combine, are prepared whereas in the second stage, the desired gel is prepared from such mixtures.
The advantage of the gel copolymer structures is that the gel may perfectly cover the lesion to be cured. Various promoting medicament forms may also be added to such gels prepared by the above process.
The polymers prepared by polycondensation are polyesters, polyamides, polyurethanes. or their mixtures. The polycondensation is carried out either with a bifunctional stericalls-hindered secondarx amine or in the presence of other bifunctional monomers. The preparation of such polymers is governed by common rules of preparation of polymers by polycondensation.
In both soluble and insoluble polymers formed by condensation, quaternary ammonium salts mazez be incorporated therein by means of suitable derivatives. The precursors must be additionally quaternized.
Description of Drawings The Fig. 1 of the draing shows an EPR spectrum of an immobilized nitroxide radical in a contact lens after oxidation w°ith hvdrogen peroxide according to Example 16.
Examples Example 1
A mixture of 80 g 2-hydroxyethyl methacrylate, 0.5 g N-(2, 2,6,6-tetramethyl-piperdin-4- yl)methacrylamide, 0.6 g ethylene glycol dimethacrylate, 0. 5 g 2,2'-azobis (2-methyl- propanenitrile) (AIBN) was heated in 1000 ml benzene at 70 °C for a period of 12 hours.
The fored polwer was extracted at room temperature with 1000 ml of benzene. The powdered polymer was agitated in a mixture water-poly (ethylene glycol) 300 (macrogolum 300), to obtain a gel of required consistency suitable for therapeutic applications.
Example' ? A polymerization mixture prepared in accordance with Example 1 and after adding 0.08 g 2-dimethylaminoethyl methacrylate was polymerized in 1000 ml benzene at a temperature of 70 OC for a period of 12 hours. The copolymer has been extracted with 1000 mi benzene and reacted with 10 nil of methyl iodide for 48 hours at room temperarlre and for another 2 days with 1000 ml benzene only. The obtained powdered polymer was dried.
Example 3 The pol « mer prepared according to Example 1 was mixed with an aqueous 4% solution of copolymer pol-[(2-hydroxyethyl methacrylate)-co-2-(methacryloyloxy)[(2-hydroxyethyl methacrylate)-co-2-(methacryloyloxy) ethyl- trimethylammonium bromide] solution so that the concentration of the ammonium salt in the obtained polymer amounted 10''g/kg.
Example 4 70 g 1-vinylpyrrolidin-2-one, 10 a 2-methoxyethyl methacrylate, 7 g N-(2, 2,6,6- tetramethyl-piperidin-4-yl)acrylamide, 0.5 g 1.1'-divinyl-3, 3'-(ethane-1,1-diyl) di (2- pyrrolidone), 0.1 g AIBN was heated in 300 ml of methanol at 60 °C for 10 hours. The obtained copolymer was extracted by ethanol and after drying was pulverized. The copolymer could be swollen in water to keep up to 67 % water content.
Example 5 A mixture of 60 g 2-(2-hydroxyethoxy)ethyl methacrylate, 3 g 2-(methacryloyloxy) ethyl -1-R6-2,2,5,5-tetramethyl-2, 5-dihydropyrrole-3-carboxylate, 0.2 g 4-vinylpyridine, 0.5 g ethylene 0.5gAIBNwasheatedin950mltolueneat72°Cfor11dimethacrylate, hours. T'e copolvmer was reacted at 25 °C with a mixture of 500 ml ethanol and 500 ml benzine and 10 ml methyl iodide for 72 hours. After removal of solvents, 250 ml
water and 250 ml poly(ethylene glycol) 300 (macrogolum 300) was added to the resulting polymer IO produce gel.
Example 6 100 g 2-hydroxyethyl methacrylate, 0.4 g ethylene glycol dimethacrylate, 1 g 2-hydroxy- 2-methyl-1-phenylpropan-1-one, 6 c,'. 2,6,6-tetramethyl-piperidin-4-yl methacylate and 0.03 g 2-dimethylaminoethvl methacrylate was allowed to polymerize on a polypropylene foil for 10 min using a number of U\~ lamps 175 W arrange in line from a distance of 18 cm. A thick foil of 1 mm was obtained which was reacted with a mixture of ethanol-acetone (1: 1) containing 0.3 % methvl iodide for 48 hours. The foil can be swollen in water to take up 36 % of water.
Example 7 100 g 2-hydroxyethyl methacrylate, 0. 4 g eth-lene glycol dimethacrylate, 1 g 2-hydroxy- gN-(2,2,6,6-tetramethylpiperidin-4-yl)methacryl-2-methyl-1-p henylpropan-1-one.6 amide was allowed to polymerize on a polypropylene foil for 10 min using a number of UV lamps 175 V-arranaed in line from a distance of 18 cm. A foil of 1 mm thickness was obtained and was extracted with 30 % ethanol. The foil could be swollen in water to take up 36 % of water. For practical use, the foil may be swollen in 50 % macrogolum 300 (see the Czech Pharmacopoeial, othewise known as poly (ethylene glycol) of molecular weight 300 for medical purposes.
Example 8 100 g 2-hydroxyetyl methacrylate, 5 g 2-acetoxyethyl methacrylate, 1-methacryloyl- 3,3,5, 5-tetramethylpiperazine, 0.5 g ethylene glycol dimethacrylate, 0.02 g 2- (methacryloyloxy) ethyl-trimethvlammonium iodide. 0.5 g AIBN in 1000 ml toluene was heated at 72 OC for 11 hours. After ex-traction with benzene and drying, the copolymer was swollen by mixing thereof with 500 ml mixture water-poly (ethylene glycol) of molecular weight 400 (1: 1) to obtain gel.
Example 9 100 g 2-hydroxyethyl methacrylate. 0.4 g ethylene glycol dimethacrylate, 1 g 2- methoxy-1,2-diphenylethanone. 6 g 2,2,6. 6-tetramethylpiperidin-4-yl acrylate, was permitted to polymerize on a polypropylene foil for 10 min-using a number of LTV lamps 175 W arrange in line at a distanc ; of 18 cm. The obtained foil, 1 mm thick, was
extracted with a mixture of ethanol-acetone (1: l). The foil was oxidized with 30% hydrogen peroxide (500 ml) so that it contained 37 % of nitroxide radicals (based on the amount of added polymerizable secondary amine). The foil can be swollen in water to take up to 36 % of water.
Example 10 A mixture of 80 g 2-hydroxyethyl methacrylate, 5 g N-{3-oxo-3-[(2,2,6,6- tetramethylpiperidin-4-yl) amino] propyl} methacrylamide, 0.6 g ethylene glycol dimethacrylate, 0.5 g 2,2'-azobis (2-methyl-propanenitrile) was heated in 1000 ml of benzene at 70 °C for 12 hours. The obtained polymer was extracted at room temperature with 1000 ml benzene and oxidized in a suspension (1000 ml benzene) by 8 g 3- chloroperbenzoic acid for 24 hours at room temperature under continuous stirring. After drying and swelling in water, the polymer contained about 35 % of water. (The content of nitroxides was 48% based on the content of the amine susceptible to oxidation).
Example 11 A mixture of 80 g 2-hydroxyethyl methacrylate, 5 g N-(2,2,6,6-tetramethylpiperidin-4- yl) methacrylamide, 0.6 g ethylene glycol dimethacrylate, 0.5 g 2,2'-azobis (2- methylpropanenitrile) was, after having been bubbled through by argon stream (10 min), dosed under inert atmosphere to molds suitable for preparation of contact lenses where the mixture was polymerized at 70 °C for 12 hours. The obtained cylinders (14 mm in diameter, 10 mm high) served as the material for production of therapeutic contact lenses by lathe cutting. After swelling in water, the lens contained 36 % of water. It could be used directly for the eye treatment.
Example 12 A mixture of 80 g 2-hydroxyethyl methacrylate, 5 g 2- (methacryloyloxy) ethyl 2,2,5,5- tetramethyl-2,5-dihydropyrrolidine-3-carboxylate, 0.6 g ethylene glycol dimethacrylate, 0.5 g 2,2'-azobis (2-methylpropanenitrile) was, after bubbling through by argon stream, (10 min) dosed under inert atmosphere into molds suitable for preparation of contact lenses where it was polymerized at 70 °C for 12 hours. The obtained cylinders (14 mm in diameter, 10 mm of high) served as material for production of therapeutic contact lenses by lathe cutting. After swelling in water, the lenses were oxidized for various time periods with a 30 % hydrogen peroxide solution (1 lens in 2 ml of the solution).
After six days of oxidation at room temperature, the lenses were used for eye treatment after laser surgery with an outstanding effect.
Example 13 A mixture of 80 g 2-hydroxyethyl methacrylate, 5 g N-(2,2,5,5-tetramethylpyrrolidin-3- yl) methacrylamide, 0.6 g ethylene glycol dimethacrylate, 0.5 g 2,2'-azobis (2- methylpropanenitrile) was heated in 1000 ml benzene at 70 °C for 12 hours. The obtained polymer was extracted at room temperature with 1000 ml benzene and oxidized in suspension in 1000 ml benzene with 8 g of 3-nitroperbenzoic acid for 24 hours at room temperature under stirring. After drying and swelling in water, it contained about 35 % of water (nitroxide content 39 %, based on the amine susceptible to oxidation).
Example 14 100 g 2-hydroxyethyl methacrylate, 0.4 g ethylene glycol dimethacrylate, 1 g 2- methoxy-1,2-diphenylethanone, 3 g 2,2,6,6-tetramethylpiperidin-4-yl methacrylate, 3 g N- (l-hydroxy-2,2,6,6-tetramethylpiperidin-4-yl) methacrylamide hydrochloride was allowed to polymerize on a polypropylene foil for 10 min using a number of UV lamp 175 W arrange in line at a distance of 18 cm. The obtained 1-mm thick foil was extracted with a mixture of ethanol-acetone (1: l). The foil, after alkalinization with a 5 % solution of sodium hydrogencarbonate (100 ml), was oxidized by 30 % hydrogen peroxide (500 ml) so that it would contain 37 % by weight of nitroxide radicals. The foil was swollen in water to take up 36 % by weight of water.
Example 15 A mixture of 60 g diethylene glycol methacrylate, 3 g 2,2,5,5-tetramethylpyrrolidin-3-yl methacrylate, 0.5 g ethylene glycol dimethacrylate, 0.5 g 2,2'-azobis (2- methylpropanenitrile) was heated in 950 ml toluene for 11 hours. The copolymer was oxidized at 25 °C with a solution of 7 g 3-chloroperbenzoic acid in 500 ml ethanol and 500 ml benzene for 2 days. After removal of the solvents, the resulting polymer was treated by adding 150 ml water and 150 ml poly (ethylene glycol) 300 to obtain gel structure. The content of nitroxides was 41 % by weight.
Example 16
100 g 2-hydroxyethyl methacrylate, 0.4 g ethylene glycol dimethacrylate, 1 g 2- methoxy-1,2-diphenylethanone, 6 g 2,2,6,6-tetramethylpiperidin-4-yl methacrylate and 0.03 g 2-dimethylaminoethyl methacrylate was polymerized on a polypropylene foil for 10 min with a number of IJV lamps 175 W arrange in line at a distance of 18 cm. The obtained 1-mm thick foil was extracted with a mixture of 3000 ml ethanol-acetone (1: 1) containing 100 ml of 30 % hydrogen peroxide for 5 days. The foil could be swollen in water to keep up 36 % by weight of water. The content of nitroxides was 15 %. Its EPR spectrum is shown in Fig. 1.
Example 17 Copolymerization of the mixture of monomers according to Example 4 in a mould led to a foil (2 mm thick) which, after having been swollen in water, was used for treatment of burons. The healing of the wound covered by the foil was shortened by approximately 5 days in comparison with a wound not treated in this manner, at that, a considerable lower amount of pus was produced.
Example 18 The copolymer prepared according to Example 2, swollen in a mixture water macrogolum 300 in a ratio of 1: 1, was applied to a pus producing wound. The healing of the wound was free of any complication.
Example 19 To a poorly accessible wound (between fmgers), the gel prepared according to Example 3 was applied. This treatment resulted in accelerated healing in comparison with conventional methods, no infection being detected.
Example 19 a Fresh excoriations were covered by the foil prepared under Example 7. Most of them was fmally healed in 3 days.
Example 20 Infecte excoriations were treated by the foil prepared according to Example 7; the foil was replace in the intervals of 2 days in dependence on the pus generation. The treatment was repeated depending on the epithelization stage, mostly 2-3 times.
Example 21 First-degree bures were covered by the foil described in Example 9. It proved to be sufficient if the surfaces were covered for 2 up 3 days. In crevices, the gel prepared according to Example 1 was applied once per day for 2-3 days. The wound was finally healed in several days without visible consequences.
Example 22 Second-degree bures were treated in a similar way. If the blisters were not injured the superficial skin need not have been removed. The bures were treated by foil rebandages prepared according to Example 7 or by application of the gel prepared under Example l, depending on their accessibility. The foil could be replace once for two days, the crevices were treated with the gel once a day. The healing process was accelerated without subsequent scars.
Example 23 Third-and fourth degree bures were covered by the foil prepared according to Example 7 for transport purposes and initial treatment.
Example 24 Minute bruises were covered by the foil prepared according to Example 9 for 2 days whereupon the lesions were found substantially healed.
Example 25 The location affecte by a sting of insect was covered by the foil prepared under Example 38. After two days healed without any effets.
Example 26 To the contact skin inflammation, the foil prepared according to Example 9 was applied.
The foil was replace once a day for a period of 2 to 3 days (or longer depending on the inflammation degree). The results were similar to those described in connection with burons. The course of healing was milder.
Example 27
Seborrhoeic dermatitis and eczema were mostly treated by the gel prepared according to Example 1 for 1 hour per day. After 3 to 4 days of the treatment, the disease was practically healed.
Example 28 Crural ulcer was covered by the foil prepared under Example 7; the foil was replace after one to two days depending on the healing degree. Sometimes, the foil had to be removed and replace by a dry bandage for certain time. Substantial improvement was observe after 3 to 4 days of application.
Example 29 Chronic skin diseases, fistulas were covered by the foil prepared under Example 6. In blistering skin diseases, the foil was replace after one to three days depending on relief upon evacuation.
Example 30 Ulcer affections of oesophagus-gastric and duodenal ulcer, Crohn disease, ulcerous colitis-the gel according to Example 1 was administered. Being non resorbable, the gel could be used for soothing of inflammation.
Example 31 Blistering skin diseases, after treatment with the gel prepared under Example 1 or a foil prepared according to Example 7 improved sensations accompanied by elimination of burning and pains were detected even if the origin of inflammation was not eliminated (for example with herpes simplex or zoster, psoriasis even with pustulous, exfoliate forms).
Example 32 Fresh excessive keloidal scars can be almost removed after application of the foil prepared according to Example 7 for a period of 10 days. The elimination of keloids was perceptible.
Example 33 Endarterial stents were covered by the foil prepared according to Example 7 to avoid the growth of atheromatosis material.
Example 34 Haemoperfusion cartridges filled with polymer beads, prepared from glycidyl methacrylate and 30% of glycol methacrylate as a crosslinking agent containing bonded 2,2,6,6-tetramethylpiperidin-4-amine through rection of the glycidyl group with the amino group, were used for removal of excess free radicals present in diseases accompanied by excessive formation of free oxygen radicals.
Example 35 Contact lenses prepared according to Example 10 were used for treatment of cornea damaged by various media and influences such as alkalis, UV radiation, mechanical abrasion, bures, chronic inflammations, post surgery complications after eye laser application. The lenses were applied for 8 hours daily with substantial improvement after one week.
Example 36 A total denture prosthesis of the upper palate was covered by a paste prepared from a mixture of the powdered polymer made under Example 5 and 2-hydroxyethyl methacrylate and after covering the prosthesis surface by separation foil (cellophane), a detailed shape of the upper palate was formed. By the action of the present W initiator, 2-hydroxy-2-methyl-1-phenylpropan-1-one (2 %), after radiation with a UV lamp 125 W from a distance of 10 cm for 12 min, a hydrophilic elastic surface forms.
Example 37 30 g of a tri-block copolymer, poly (ethylene glycol)-poly (propylene glycol)- poly (ethylene glycol) (molecular weight 3000), 33 g bis (4-isocyanatocyklohexyl) methane, 0.5 g 4-hydroxy-2,2,6,6-tetramethylpiperideine-1-oxyl, 03 g poly (vinyl alcool) and 0.8 g 1,4-diazabicyklo [2.2.2] octane were mixed and poured on a polyester foil. On heating with an infrared lamp at 40 °C for 2 hours, a desired film was formed.
Example 38 A mixture of 15 g poly (propylene oxide) (molecular weight 1500), 2.1 g hexane-1,6- diyl diisocyanate, 0.7 g 2-ethyl-2 (hydroxymethyl) propane-1,3-diol, 0.5 g 3- (2- hydroxyethyl)-2,2,5,5-tetramethylpyrrolidin-1-yloxyl, 0.1 g 3-diethylaminopropylamine was poured on a hydrophobized glass and heated at 35 OC for 2 hours. A hydrophilic foil
was obtained which was extracted by a mixture of 200 ml ethanol and 10 ml methyl iodide for 2 days. Extraction with 500 mi mixture ethanol-water followed.
Example 39 A hydrophilic contact lens was produced by lathe cutting of a block prepared by block polymerization of 2-hydroxyethyl methacrylate with 0.3 % glycol dimethacrylate under standard polymerization conditions. Its surface was modifie by the rection of 3- isocyanato-2,2,5,5-tetramethylpyrrolidin-1-yloxyl with hydrophilic groups of the contact lens in a 1,2-dimethoxyethane solution. The present radical was then partly reduced to hydroxylamine with hydrogen under the overpressure of 100 mm water column and catalysis by a platinum net.
Example 40 A homopolymer prepared by anionic polymerization of 4-methacryloyloxy-2,2,6,6-tetra- methyl (piperidin-1-yloxyl (molecular weight 2600) was dissolve in an ethanolic solution of poly (2-hydroxyethyl) methacrylate and a foil was cast from the solution. The foil was used for comparison for treatment of a burn at forearm. The therapeutic effect was substantially better in comparison with conventional methods.
Example 41 The ester prepared from poly (ethylene glycol) monoethyl ether (molecular weight 600) and 2,2,5,5-tetramethyl-2,5-dihydropyrrole-3-carboxylic acid was used as a 3 % (by weight) admixture in polycondensation of a block copolymer poly (ethylene glycol)- poly (propylene glycol) (molecular weight 800) with hexan-1,6-diyl diisocyanate. The polymer was obtained as a foil, which was, after swelling in a mixture water- macrogolum 300, applied to bed-sores caused by long staying in bed. The results were substantially better than those obtained by conventional methods.
Example 42 Poly (ethylene glycol) (molecular. weight 3000), with carboxylic acid end groups, was converted to diamide by the rection with 4-amino-2,2,6,6-tetramethylpiperidine using dicyclohexylcarbodiimide. This polymer served as a 5 % ingredient in the radical polymerization of 2-hydroxyethyl methacrylate in a mould to obtain a 2-mm thick foil.
The foil was successfully used for treatment of crural ulcers.
Industrial applicability The preparation according to the invention is widely applicable for prevention and healing of inflammation diseases, surface injuries of skin, hide, fascia and muscle and lesions extending to various depths which are accompanied by a massive production of radicals by the oxygen reduction under the formation of reactive oxygen products.
The preparation is applicable in sanitary, hospital and post hospital care and can be added to all preparations used as first aid means for the said types of lesion.