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DK175288B1 - Pharmaceutical agents containing drugs which are unstable or sparingly soluble in water, and methods for their preparation - Google Patents

Pharmaceutical agents containing drugs which are unstable or sparingly soluble in water, and methods for their preparation Download PDF

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DK175288B1
DK175288B1 DK198503595A DK359585A DK175288B1 DK 175288 B1 DK175288 B1 DK 175288B1 DK 198503595 A DK198503595 A DK 198503595A DK 359585 A DK359585 A DK 359585A DK 175288 B1 DK175288 B1 DK 175288B1
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water
cyclodextrin
drug
agent according
methyl
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Ulrich Brauns
Bernhard Willi Werner Mueller
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Janssen Pharmaceutica Nv
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    • BPERFORMING OPERATIONS; TRANSPORTING
    • B82NANOTECHNOLOGY
    • B82YSPECIFIC USES OR APPLICATIONS OF NANOSTRUCTURES; MEASUREMENT OR ANALYSIS OF NANOSTRUCTURES; MANUFACTURE OR TREATMENT OF NANOSTRUCTURES
    • B82Y5/00Nanobiotechnology or nanomedicine, e.g. protein engineering or drug delivery
    • AHUMAN NECESSITIES
    • A61MEDICAL OR VETERINARY SCIENCE; HYGIENE
    • A61KPREPARATIONS FOR MEDICAL, DENTAL OR TOILETRY PURPOSES
    • A61K47/00Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient
    • A61K47/50Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient the non-active ingredient being chemically bound to the active ingredient, e.g. polymer-drug conjugates
    • A61K47/69Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient the non-active ingredient being chemically bound to the active ingredient, e.g. polymer-drug conjugates the conjugate being characterised by physical or galenical forms, e.g. emulsion, particle, inclusion complex, stent or kit
    • A61K47/6949Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient the non-active ingredient being chemically bound to the active ingredient, e.g. polymer-drug conjugates the conjugate being characterised by physical or galenical forms, e.g. emulsion, particle, inclusion complex, stent or kit inclusion complexes, e.g. clathrates, cavitates or fullerenes
    • A61K47/6951Medicinal preparations characterised by the non-active ingredients used, e.g. carriers or inert additives; Targeting or modifying agents chemically bound to the active ingredient the non-active ingredient being chemically bound to the active ingredient, e.g. polymer-drug conjugates the conjugate being characterised by physical or galenical forms, e.g. emulsion, particle, inclusion complex, stent or kit inclusion complexes, e.g. clathrates, cavitates or fullerenes using cyclodextrin
    • CCHEMISTRY; METALLURGY
    • C08ORGANIC MACROMOLECULAR COMPOUNDS; THEIR PREPARATION OR CHEMICAL WORKING-UP; COMPOSITIONS BASED THEREON
    • C08BPOLYSACCHARIDES; DERIVATIVES THEREOF
    • C08B37/00Preparation of polysaccharides not provided for in groups C08B1/00 - C08B35/00; Derivatives thereof
    • C08B37/0006Homoglycans, i.e. polysaccharides having a main chain consisting of one single sugar, e.g. colominic acid
    • C08B37/0009Homoglycans, i.e. polysaccharides having a main chain consisting of one single sugar, e.g. colominic acid alpha-D-Glucans, e.g. polydextrose, alternan, glycogen; (alpha-1,4)(alpha-1,6)-D-Glucans; (alpha-1,3)(alpha-1,4)-D-Glucans, e.g. isolichenan or nigeran; (alpha-1,4)-D-Glucans; (alpha-1,3)-D-Glucans, e.g. pseudonigeran; Derivatives thereof
    • C08B37/0012Cyclodextrin [CD], e.g. cycle with 6 units (alpha), with 7 units (beta) and with 8 units (gamma), large-ring cyclodextrin or cycloamylose with 9 units or more; Derivatives thereof
    • C08B37/0015Inclusion compounds, i.e. host-guest compounds, e.g. polyrotaxanes

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  • Health & Medical Sciences (AREA)
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  • Pharmacology & Pharmacy (AREA)
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  • Crystallography & Structural Chemistry (AREA)
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  • Pharmaceuticals Containing Other Organic And Inorganic Compounds (AREA)
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  • Medicines That Contain Protein Lipid Enzymes And Other Medicines (AREA)
  • Acyclic And Carbocyclic Compounds In Medicinal Compositions (AREA)

Abstract

Novel pharmaceutical compositions comprise inclusion compounds of drugs, which are instable or only sparingly soluble in water, with partially etherified beta -cyclodextrin derivatives having hydroxyalkyl and optionally additional alkyl groups.

Description

DK 175288 B1DK 175288 B1

Opfindelsen angår farmaceutiske midler indeholdende lægemidler, der er ustabile eller kun sparsomt opløselige i vand, og fremgangsmåder til deres fremstilling. Midlerne er karakteristiske ved forøget vandopløselighed og forbedret stabilitet.The invention relates to pharmaceutical agents containing drugs which are unstable or only sparingly soluble in water, and methods for their preparation. The agents are characterized by increased water solubility and improved stability.

5 Et stort antal lægemidler er kun dårligt opløselige eller sparsomt opløselige i vand, så- i ledes at egnede applikationsformer, såsom dryppeopløsninger eller injektionsopløsninger fremstilles under anvendelse af andre polære additiver, såsom propylenglycol osv.A large number of drugs are only poorly soluble or sparingly soluble in water, so that suitable application forms such as drip solutions or injection solutions are prepared using other polar additives such as propylene glycol, etc.

Hvis lægemiddelmolekylet har basiske eller sure grupper, er der den yderligere mulighed at forøge vandopløseligheden ved saltdannelse. Som regel fører dette til formind- 10 sket effektivitet eller tab af kemisk stabilitet. På grund af den forskudte fordelingsligevægt er det muligt, at lægemidlet kun langsomt gennemtrænger den lipofile membran, svarende til koncentrationen af den ikke-dissocierede fraktion, medens den ioniske fraktion kan undergå hurtig hydrolytisk dekomponering.If the drug molecule has basic or acidic groups, there is the further possibility of increasing the water solubility by salt formation. As a rule, this leads to diminished efficiency or loss of chemical stability. Because of the offset equilibrium, it is possible that the drug only slowly penetrates the lipophilic membrane, corresponding to the concentration of the undissociated fraction, while the ionic fraction can undergo rapid hydrolytic decomposition.

15 Yderligere "vandagtige" opløsningsmidler, såsom lavmolekulære polyethylenglycoler eller 1,2-propylenglycol anvendes derfor til fremstilling af vandige opløsninger af sparsomt vandopløselige lægemidler, hvilke glycoler dog ikke kan betragtes som farmakologisk indifferente, eller lægemidlet opløseliggøres under anvendelse af overfladeaktive midler, således at lægemiddelmolekyleme okkluderes i miceller. Denne opløseliggørel- 20 se har talrige ulemper: molekylerne af det anvendte overfladeaktive middel har hyppigt en stærkt hæmolytisk virkning og lægemidlet skal ud af micellen ved diffusion efter applikationen. Dette resulterer i en forhalet virkning (jf. B. W. Muller, Gelbe Reihe, bind X, side 132 ff (1983)).Further "aqueous" solvents such as low molecular weight polyethylene glycols or 1,2-propylene glycol are therefore used to prepare aqueous solutions of sparingly water-soluble drugs, which, however, cannot be considered pharmacologically inert or the drug is solubilized using surfactants, occluded in micelles. This solubility has numerous drawbacks: the molecules of the surfactant used frequently have a strong hemolytic effect and the drug has to leave the micelle upon diffusion after application. This results in a delayed effect (cf. B. W. Muller, Gelbe Reihe, Vol. X, p. 132 et seq. (1983)).

25 Det kan derfor siges, at der ikke eksisterer nogen tilfredsstillende og generelt anvendelig fremgangsmåde til opløseliggørelse.25 It can therefore be said that there is no satisfactory and generally applicable solubilization process.

Til faste lægemidler er det også vigtigt at gøre det sparsomt vandopløselige lægemiddel vandopløseligt, fordi en god opløselighed forøger biotilgængeligheden af lægemidlet.For solid drugs, it is also important to make the sparingly water-soluble drug water-soluble, because good solubility increases the bioavailability of the drug.

30 Det er blevet beskrevet, at inklusionsforbindelser, f.eks. med urinstof eller komplekser af polyvinylpyrrolidon kan forbedre opløseligheden af en forbindelse, men i vandig op-It has been described that inclusion compounds, e.g. with urea or complexes of polyvinylpyrrolidone can improve the solubility of a compound but in aqueous solution.

I DK 175288 B1 II DK 175288 B1 I

i 2 Ii 2 I

I løsning er de ikke stabile. Sådanne inklusionsforbindelser er derfor bedst egnede til fa- IIn solution, they are not stable. Such inclusion compounds are therefore best suited for use in phases

I ste applikationsformer af lægemidler. IIn first application forms of pharmaceuticals. IN

I Dette er anderledes, når der anvendes Οί-, β- og γ-cyclodextrin, som kan binde et læge- IThis is different when Οί-, β- and γ-cyclodextrin is used, which can bind a physician.

I 5 middel i sin ring, også i vandig opløsning (W. Sanger, Angewandte Chemie 92, 343 IIn 5 medium in its ring, also in aqueous solution (W. Sanger, Angewandte Chemie 92, 343 I

I (1980)) Det er imidlertid en ulempe, at β-cyclodextrinet selv kun er dårligt vandopløse- - II (1980)) However, it is a disadvantage that the β-cyclodextrin itself is only poorly water-soluble.

I ligt (1,8 g pr. 100 ml), således at de terapeutisk nødvendige lægemiddelkoncentrationer II corpus (1.8 g per 100 ml) so that the therapeutically needed drug concentrations I

I ikke opnås. IYou are not achieved. IN

I 10 Hvis der dannes et derivat af cyclodextrinet, kan dets opløselighed og derfor mængden IIf a derivative of the cyclodextrin is formed, its solubility and therefore the amount of I

I af opløst lægemiddel forøges betydeligt. Tysk offentliggørelsesskrift 31 18 218 beskri- IThe dissolved drug increases significantly. German Publication Publication 31 18 218 Description

I ver således en opløseliggørelsesmetode under anvendelse af methyleret /3-cyclodextrin IThus, a solubilization method is employed using methylated β-cyclodextrin I

I som monomethylderivat med 7 methylgrupper og især som dimethylderivat med 14 II as monomethyl derivative with 7 methyl groups and especially as dimethyl derivative with 14 L

I methylgrupper. Med 2,6-di-Omethylderivatet er det f.eks. muligt at forøge vandoplø- IIn methyl groups. With the 2,6-di-Omethyl derivative, e.g. possible to increase water dissolution

I 15 seligheden af indometacin 20,4 gange og vandopløseligheden af digitoxin 81,6 gange. IIn the solubility of indomethacin 20.4 times and the water solubility of digitoxin 81.6 times. IN

I E. Fenyvesi et al. (Proceedings of the first International Symposium on Cyclodextrins; IIn E. Fenyvesi et al. (Proceedings of the first International Symposium on Cyclodextrins; I

I Budapest 1981, side 345-356) beskriver fremstillingen af cyclodextrin-polymerer ved IIn Budapest 1981, pages 345-356) describe the preparation of cyclodextrin polymers by I

I omsætning med epichlorhydrin, som udviser en høj vandopløselighed og egner sig til IIn reaction with epichlorohydrin, which exhibits a high water solubility and is suitable for I

I 20 forhøjelse af opløseligheden i vand af svært opløselige forbindelser. Polymererne bliver IIn increasing the solubility in water of highly soluble compounds. The polymers become you

I fremstillet af monomeret β- og γ-cyclodextrin, og de til anvendelse udvalgte polymerer II made of monomeric β- and γ-cyclodextrin and the polymers selected for use I

I besidder en gennemsnitlig molekylevægt fra 4000 til 6000, med en middel-molekyle- IYou have an average molecular weight of 4000 to 6000, with an average molecular I

I vægt Mw på 5300. IIn weight Mw of 5300. I

I 25 IWO-A-820051 bliver indkapslede forbindelser af retinoider med cyclodextrin og eye- IIn IWO-A-820051, encapsulated compounds of cyclodextrin and eye retinoids

I lodextrinderivater beskrevet. Det tilgrundliggénde problem i skriftet er nedsættelsen af IIn lodextrin derivatives described. The fundamental problem in writing is the reduction of I

I de toksiske bivirkninger af retinoider gennem modifikation af den molekylære struktur IIn the toxic side effects of retinoids through modification of the molecular structure I

I og/eller kompleksdannelse med cyclodextriner. Fedtopløseligheden af substanserne IIn and / or complexation with cyclodextrins. The fat solubility of the substances I

I skal formindskes, og dermed bliver deres tilbøjelighed til koncentrering i fedtvæv ned- IYou need to decrease, and thus their propensity for concentration in adipose tissue decreases

I 30 sat eller undgået. I skriftet bliver a-, β- og γ-cyclodextriner såvel som deres derivater IIn 30 set or avoided. In the specification, α-, β- and γ-cyclodextrins as well as their derivatives I

I betegnet som lige egnede til kompleksdannelsen, mens der som eneste eksempel som IYou designate as equally suitable for complex formation, while as the only example like I

DK 175288 B1 3 anvendelige derivater i første linie nævnes methoxyderivater af α-, β- og γ-cyclodex-trin.Applicable first-line derivatives are mentioned methoxy derivatives of α, β and γ-cyclodex steps.

Til terapeutisk brug udviser methylderivateme af /3-cyclodextrin imidlertid ulemper, på 5 grund af deres forøgede lipofilitet har de en hæmolytisk virkning, og de forårsager endvidere irritationer af slimhinden og øjnene. Deres akutte intravenøse toxicitet er endnu højere end den allerede betydelige toxicitet af det usubstituerede Ø-cyclodextrin. Det er en yderligere alvorlig ulempe for den praktiske anvendelse, at opløseligheden af dime-thyl-j3-cyclodextrin og dets komplekser undergår et brat fald ved højere temperaturer, 10 således at krystallinsk dextrin udfælder ved opvarmning. Dette fænomen gør det meget vanskeligt at sterilisere opløsningerne ved de sædvanlige temperaturer på 100 til 121°C.However, for therapeutic use, the methyl derivatives of β-cyclodextrin exhibit disadvantages, because of their increased lipophilicity, they have a haemolytic effect and further cause irritation of the mucosa and eyes. Their acute intravenous toxicity is even higher than the already significant toxicity of the unsubstituted β-cyclodextrin. It is a further serious disadvantage of the practical application that the solubility of dimethyl-3-cyclodextrin and its complexes undergoes a sharp decrease at higher temperatures, so that crystalline dextrin precipitates upon heating. This phenomenon makes it very difficult to sterilize the solutions at the usual temperatures of 100 to 121 ° C.

Overraskende har det nu vist sig, at visse andre j3-cyclodextrinderivater kan danne in-15 klusionsforbindelser, som også betydeligt forøger vandopløseligheden af sparsomt vandopløselige og ustabile lægemidler uden at have de ovenfor beskrevne ulemper.Surprisingly, it has now been found that certain other β-cyclodextrin derivatives can form inclusion compounds which also significantly increase the water solubility of sparsely water-soluble and unstable drugs without the disadvantages described above.

Opfindelsen angår derfor hidtil ukendte farmaceutiske midler omfattende inklusionsforbindelser af kun sparsomt vandopløselige eller i vand ustabile lægemidler med et 20 delvis forethret /S-cyclodextrin, hvor ethersubstituenten er hydroxyethyl-, hydroxypro-pyl-, eller dihydroxypropylgrupper, hvorved en del af ethersubstituenteme om nødvendigt kan være methyl- eller ethylgrupper og /3-cyclodextrinetheren udviser en vandop-løselighed på mere end 1,8 g i 100 ml vand, hvorved indkapslingsforbindelser af reti-noider med jS-cyclodextrinethere, for så vidt deres ethersubstituenter er methyl-, ethyl-25 og 2-hydroxyethylgrupper, samt indkapslingsforbindelser af sparsomt vandopløselige eller i vand ustabile lægemidler med blandinger af jS-cyclodextrin-epichlorhydrin-deri-vater med en middelmol ekylevægt Mw, er undtagetThe invention therefore relates to novel pharmaceutical agents comprising inclusion compounds of only sparingly water-soluble or water-unstable drugs with a partially etherified / S-cyclodextrin, wherein the ether substituent is hydroxyethyl, hydroxypropyl, or dihydroxypropyl groups, whereby some of be methyl or ethyl groups and the β-cyclodextrin ether exhibits a water solubility of more than 1.8 g in 100 ml of water, thereby encapsulating compounds of retinoids with β-cyclodextrin ethers insofar as their ether substituents are methyl, ethyl-25 and 2-hydroxyethyl groups, as well as encapsulating compounds of sparingly water-soluble or water-unstable drugs with mixtures of β-cyclodextrin-epichlorohydrin derivatives having a medium molecular weight Mw are excluded

Brugen af delvis methylerede j3-cyclodextrinethere med 7 til 14 methyl grupper i /?-cyc-30 lodextrinmolekylet, således som de er kendt fra DE-A-31 18 218, falder ikke ind under den foreliggende opfindelse. Endvidere er indkapslingsforbindelser af retinoider medThe use of partially methylated β-cyclodextrin ethers with 7 to 14 methyl groups in the β-cyclodextrin molecule, as known from DE-A-31 18 218, does not fall within the scope of the present invention. Furthermore, encapsulating compounds of retinoids are included

I DK 175288 B1 II DK 175288 B1 I

I 4 II 4 I

I /3-cyclodextrinethere ifølge opfindelsen, så vidt deres ethersubstituenter er methyl-, II / 3-cyclodextrin ethers of the invention insofar as their ether substituents are methyl,

I ethyl- og 2-hydroxyethylgrupper (jf. WO-A-820051), og indkapslingsforbindelser af IIn ethyl and 2-hydroxyethyl groups (cf. WO-A-820051), and encapsulating compounds of I

I sparsomt vandopløselige eller i vand ustabile lægemidler med blandinger af /3-cyclo- IIn sparingly water-soluble or water-unstable drugs with mixtures of / 3-cyclo-I

I dextrin-epichlorhydrin-derivater med en middelmolekylevægt Mw 5300, udeladt. IIn dextrin epichlorohydrin derivatives with a mean molecular weight Mw 5300, omitted. IN

I 5 II 5 I

I /3-cyclodextrin er en forbindelse med en ringstruktur, bestående af 7 anhydroglucoseen- , II / 3-cyclodextrin is a compound having a ring structure consisting of 7 anhydroglucose

I heder. Det omtales også som cycloheptaamylose. Hver af de 7 glucoseringe indeholder IIn honor. It is also referred to as cycloheptaamylose. Each of the 7 glucosings contains I

I i 2-, 3-, og 6-stillingen tre hydroxygrupper, der kan være forethrede. I de delvis for- IIn the 2, 3, and 6 positions, three hydroxy groups may be etherified. In the partially for- I

I ethrede /5-cyclodextrinderivater, der anvendes ifølge opfindelsen, er kun en del af disse IIn etherated / 5-cyclodextrin derivatives used according to the invention, only part of these

I 10 hydroxygrupper forethret med de angivne hydroxyalkylrester, samt endvidere i givet IIn 10 hydroxy groups etherified with the indicated hydroxyalkyl residues, as well as in given I

I fald forethret med methyl- eller ethylestere. Når de er forethret med 5-hydroxyalkylre- IIn cases etherified with methyl or ethyl esters. When etherified with 5-hydroxyalkyl radical

I ster, hvilket kan udføres ved omsætning med egnede alkylenoxider, anføres substituti- ISubstances which can be carried out by reaction with suitable alkylene oxides are substituted

I onsgraden som molær substitutionsgrad (MS), nemlig i mol alkylenoxid pr. anhydro- IIn the degree of molar substitution degree (MS), namely in moles of alkylene oxide per anhydro-I

I glucoseenhed, jf. US-A-34 59 731, spalte 4. Ved hydroxyalkylethere af /3-cyclodextrin, IIn glucose unit, cf. US-A-34 59 731, column 4. For hydroxyalkyl ethers of / 3-cyclodextrin, I

I 15 der anvendes ifølge opfindelsen, er den molære substitutionsgrad mellem 0,2 og 10, IIn the present invention, the molar degree of substitution is between 0.2 and 10.1

I fortrinsvis mellem 0,2 og 2. Særligt foretrukket er en molær substitutionsgrad på ca. IPreferably between 0.2 and 2. Particularly preferred is a degree of molar substitution of approx. IN

I 0,25 til ca. 1. IFor 0.25 to approx. 1. I

I Forethringen med alkylgrupper kan angives direkte som substitutionsgrad (DS) pr. glu- IIn the etherification with alkyl groups can be stated directly as degree of substitution (DS) per glu- I

I 20 coseenhed, der som ovenfor nævnt er 3 ved fuldstændig substitution. Der anvendes del- IIn 20 unit of unit, as mentioned above, 3 is at complete substitution. Part I is used

I vis forethrede /3-cyclodextriner ifølge opfindelsen, som foruden hydroxyalkylgrupper IIn some etherated β-cyclodextrins of the invention, which, in addition to hydroxyalkyl groups I

I også omfatter alkylgrupper, især methyl- eller ethylgrupper op til en substitutionsgrad IYou also include alkyl groups, especially methyl or ethyl groups up to a degree of substitution I

på fra 0,2 til 2,0, fortrinsvis fra 0,2 til 1,5. Mest hensigtsmæssigt er substitutionsgraden Iof from 0.2 to 2.0, preferably from 0.2 to 1.5. Most suitable is the degree of substitution I

I med alkylgrupper mellem ca. 0,5 og ca. 1,2. II with alkyl groups between ca. 0.5 and approx. 1.2. IN

I 25 II 25 I

I Det molære forhold mellem lægemiddel og /3-cyclodextrinether er fortrinsvis ca. 1:6 til IPreferably, in the molar ratio of drug to β-cyclodextrin ether, approx. 1: 6 to 1

I 4:1, især ca. 1:2 til 1:1. Som regel foretrækkes det at anvende det kompleksdannende IIn 4: 1, especially approx. 1: 2 to 1: 1. As a rule, it is preferred to use the complexing I

I middel i et molært overskud. IIn the mean in a molar excess. IN

I 30 Nyttige kompleksdannende midler er især hydroxyethyl-, hydroxypropyl- og dihydro- IIn particular, useful complexing agents are hydroxyethyl, hydroxypropyl and dihydro-I

I xypropyletheren, deres tilsvarende blandede ethere og yderligere blandede ethere med IIn the xypropyl ether, their corresponding mixed ethers and further mixed ethers with I

5 DK 175288 B1 methyl- eller ethylgrupper, såsom methyl-hydroxyethyl-, methyl-hydroxypropyl-, ethylhydroxyethyl- og ethyl-hydroxypropylether af /3-cyclodextrin.Methyl or ethyl groups such as methyl hydroxyethyl, methyl hydroxypropyl, ethyl hydroxyethyl and ethyl hydroxypropyl ether of β-cyclodextrin.

Fremstillingen af hydroxyalkyletheme af /3-cyclodextrin kan udføres ved anvendelse af 5 fremgangsmåden ifølge US patent nr. 3.459.731. Egnede fremstillingsmåder til /3-cyc-lodextrinethere kan yderligere findes i J. Szejtli med flere, Stårke 32, 165 (1980) og A.P. Croft og R.A. Bartsch, Tetrahedron 39, 1417 (1983). Blandede ethere af /S-cyclo-dextrin kan fremstilles ved reaktion af /3-cyclodextrin i et basisk flydende reaktionsmedium omfattende en alkalimetalhydroxid, vand og eventuelt mindst et organisk opløs-10 ningsmiddel, (f.eks. dimethoxyethan eller ispopropanol) med mindst to forskellige hy-droxyalkyleringsmidler og eventuelt alkylerende forethrende midler (f. eks, ethyleno-xid, propylenoxid, methyl- eller ethylchlorid).The preparation of the hydroxyalkyl ethers of β-cyclodextrin can be carried out using the method of US Patent No. 3,459,731. Suitable methods of preparation for β-cyclodextrin ethers can be further found in J. Szejtli et al., Starkke 32, 165 (1980) and A.P. Croft and R.A. Bartsch, Tetrahedron 39, 1417 (1983). Mixed ethers of β-cyclodextrin may be prepared by reaction of β-cyclodextrin in a basic liquid reaction medium comprising an alkali metal hydroxide, water and optionally at least one organic solvent (e.g. dimethoxyethane or isopropanol) with at least two various hydroxyalkylating agents and optionally alkylating etherifying agents (e.g., ethylene oxide, propylene oxide, methyl or ethyl chloride).

Lægemidler, der udviser henholdsvis en betydelig forøget vandopløselighed og forbed-15 ret stabilitet efter at være omdannet til inklusionsforbindelser med ovennævnte /3-cyclo-dextrinethere, er de, der har den nødvendige form og størrelse, dvs. som passer ind i hulheden i /3-cyclodextrinringsystemet. Dette indbefatter f.eks. ikke-steroide antirheu-matiske midler, steroider, hjerteglycosider, og derivater af benzodiazepin, benzimida-zol, piperidin, piperazin, imidazol eller triazol.Drugs that exhibit significantly increased water solubility and improved stability, respectively, after being converted to inclusion compounds with the above-mentioned 3-cyclodextrin ethers, are those having the necessary shape and size, i. which fits into the cavity of the / 3-cyclodextrin ring system. This includes e.g. non-steroidal antirheumatic agents, steroids, cardiac glycosides, and derivatives of benzodiazepine, benzimidazole, piperidine, piperazine, imidazole or triazole.

2020

Nyttige benzimidazolderivater er thiabendazol, fuberidazol, oxibendazol, parbendazol, cambendazol, mebendazol, fenbendazol, flubendazol, albendazol, oxfendazol, nocoda-zol og astemisol. Egnede piperadinderivater er fluspirilen, pimozid, penfluridol, lope-ramid, astemizol, ketanserin, levocabastin, cisaprid, altanserin og ritanserin. Egnede pi-25 perazinderivater indbefatter lidoflazin, flunarizin, mianserin, oxatomid, mioflazin og cinnarizin. Eksempler på egnede imidazolderivater er metronidazol, omidazol, iproni-dazol, tinidazol, isoconazol, nimorazol, burimamid, metiamid, metomidat, enilconazol, etomidat, econazol, clotrimazol, camidazol, cimetidin, docodazol, sulconazol, parcona-zol, orconazol, butoconazol, triadiminol, tioconazol, valconazol, fluotrimazol, ketoco-30 nazol, oxiconazol, lombazol, bifonazol, oxmetidin, fenticonazol og tubulazol. Som egnede triazolderivater kan nævnes virazol, itraconazol og terconazol.Useful benzimidazole derivatives are thiabendazole, fuberidazole, oxybendazole, parbendazole, cambendazole, mebendazole, fenbendazole, flubendazole, albendazole, oxfendazole, nocodazole and astemisole. Suitable piperadine derivatives are fluospiril, pimozide, penfluridol, lope-ramide, astemizole, ketanserin, levocabastine, cisapride, altanserin and ritanserin. Suitable piperazine derivatives include lidoflazine, flunarizine, mianserin, oxatomide, myoflazine and cinnarizine. Examples of suitable imidazole derivatives are metronidazole, omidazole, ipronidazole, tinidazole, isoconazole, nimorazole, burimamide, methiamide, metomidate, enilconazole, etomidazole, econazole, clotrimazole, camidazole, cimetidine, cimetidine, cimetidine, , thioconazole, valconazole, fluotrimazole, ketoconazole, oxiconazole, lombazole, bifonazole, oxmetidine, fenticonazole and tubulazole. Suitable triazole derivatives include virazole, itraconazole and terconazole.

I DK 175288 B1 II DK 175288 B1 I

I 6 II 6 I

I Særligt værdifulde farmaceutiske midler fås ved omdannelse af etomidat, ketoconazol, IParticularly valuable pharmaceutical agents are obtained by conversion of etomidate, ketoconazole, I

I tubulazol, itraconazol, levocabastin eller flunarizin til en vandopløselig form under an- IIn tubulazole, itraconazole, levocabastine or flunarizine, in a water-soluble form under

I vendelse af de kompleksdannende midler ifølge opfindelsen. Sådanne farmaceutiske ITurning on the complexing agents of the invention. Such pharmaceutical I

I midler er der for særlig genstand for den foreliggende opfindelse. IIn particular, there is a particular object of the present invention. IN

I 5 II 5 I

I Opfindelsen angår endvidere en fremgangsmåde til fremstilling af farmaceutiske midler IThe invention also relates to a process for the preparation of pharmaceutical agents I

I af sparsomt vandopløselige eller vandustabile lægemidler, som er ejendommelig ved II of sparingly water-soluble or water-unstable drugs which are peculiar to I

I opløsning af j3-cyclodextrinetheren i vand og tilsætning dertil af det udvalgte lægemid- IIn solution of the β-cyclodextrin ether in water and addition thereto of the selected drug.

I del, samt eventuelt tørring af opløsningen af den dannede inklusionsforbindelse under IIn part, and optionally drying the solution of the inclusion compound formed under I

I 10 anvendelse af i og for sig kendte måder. Dannelsen af opløsningen kan ske ved tempe- IIn the use of methods known per se. The formation of the solution can take place at temp

I raturer mellem 15 og 35°C. IAt temperatures between 15 and 35 ° C. IN

I Lægemidlet tilsættes hensigtsmæssigt portionsvis. Vandet kan yderligere omfatte fysio- IThe portion of the drug is conveniently added portionwise. The water may further comprise physical

I logisk forenelige forbindelser, såsom natriumchlorid, kaliumnitrat, glucose, mannit, IIn logically compatible compounds such as sodium chloride, potassium nitrate, glucose, mannite, I

I 15 sorbit, xylit eller stødpuder, såsom phosphat, acetat eller citratstødpude. IIn sorbit, xylite or buffer such as phosphate, acetate or citrate buffer. IN

I Under anvendelse af /3-cyclodextrinethere ifølge opfindelsen er det muligt at fremstille II Using β-cyclodextrin ethers according to the invention, it is possible to prepare I

I applikationsformer af lægemidler til oral, parenteral eller topisk applikation, f.eks. infil- IIn application forms of drugs for oral, parenteral or topical application, e.g. infil- I

I sions- og injektionsopløsninger, dryppeopløsninger (f.eks. øjendråber eller næsedrå- IIn solution and injection solutions, drip solutions (eg eye drops or nasal drops)

I 20 ber), sprøjtevæsker, aerosoler, sirupper og medicinske bade. IIn 20 ber), spray fluids, aerosols, syrups and medical baths. IN

I De vandige opløsninger kan yderligere omfatte egnede fysiologisk anvendelige konser- IThe aqueous solutions may further comprise suitable physiologically useful concentrates

I veringsmidler, såsom kvatemære ammoniumsæber eller chlorbutanol. IIn preservatives such as quaternary ammonium soaps or chlorobutanol. IN

I 25 Til fremstilling af faste præparater bliver opløsningerne af inklusionsforbindelseme tør- IFor the preparation of solid compositions, the solutions of the inclusion compounds become dry

I ret ved anvendelse af sædvanlige metoder. Vandet kan således fordampes i en rotati- IIn court using usual methods. Thus, the water can be evaporated in a rotary I

I onsfordamper eller ved lyofilisering. Remanensen pulveriseres og eventuelt efter til- IIn evaporator or lyophilization. The residue is pulverized and optionally after addition

I sætning af yderligere indifferente bestanddele bliver den omdannet til ubelagte eller be- IIn addition of additional inert constituents, it is transformed into uncoated or coated

I lagte tabletter, suppositorier, kapsler, cremer eller salver. IIn laid tablets, suppositories, capsules, creams or ointments. IN

I 30 II 30 I

7 DK 175288 B17 DK 175288 B1

De følgende eksempler tjener til at illustrere opfindelsen, som dog ikke er begrænset til eksemplerne.The following examples serve to illustrate the invention, but not limited to the examples.

Phosphatstødpudeopløsningen, der er nævnt i eksempler, havde en pH-værdi på 6,6 og 5 følgende sammensætning: KH2P04 68,05 gThe phosphate buffer solution mentioned in Examples had a pH of 6.6 and 5 of the following composition: KH2PO4 68.05 g

NaOH 7,12 gNaOH 7.12 g

Aqua demin.ad. 5000,0 g 10Aqua demin.ad. 5000.0 g 10

Alle procenter er vægtprocenter.All percentages are weight percentages.

Eksempel 1 15 Gående ud fra en 7% stamopløsning af hydroxyethyl /3-cyclodextrin (MS 0,43) i phos-phatstødpudeopløsning blev der fremstillet en fortyndingsrække, således at koncentrationen af kompleksdannende middel blev forøget trinvis 1% 3 ml af disse opløsninger blev pipetteret i 5 ml glas med afbrækkelig top indeholdende lægemiddel, der skulle afprøves. Efter rystning i 24 timer ved 25°C, blev opløsningen filtreret gennem et 20 membranfilter (0,22 mikron) og det opløste lægemiddelindhold blev bestemt spektrofo-tometrisk. Fig. 1, 3 og 4 viser forøgelsen i lægemiddelkoncentration i opløsning i forhold til koncentrationen af det kompleksdannende middel for indometacin (fig. 1), piro-xicam (fig. 3) og diazepam (fig. 4). Den maksimale lægemiddelkoncentration er begrænset af mætningsopløseligheden af cyclodextrinderivatet i stødpuden som, hvor det 25 drejer sig om hydroxyethyl-/3-cyclodextrin (MS 0,43) nås ved 7,2 g pr. 100 ml.Example 1 Starting from a 7% stock solution of hydroxyethyl / 3-cyclodextrin (MS 0.43) in phosphate buffer pad, a dilution series was prepared so that the concentration of complexing agent was incrementally increased by 1% 3 ml of these solutions. in 5 ml glass with removable top containing drug to be tested. After shaking for 24 hours at 25 ° C, the solution was filtered through a 20 membrane filter (0.22 micron) and the dissolved drug content was determined spectrophotometrically. FIG. Figures 1, 3 and 4 show the increase in drug concentration in solution relative to the concentration of the complexing agent for indomethacin (Fig. 1), pyroxicam (Fig. 3) and diazepam (Fig. 4). The maximum drug concentration is limited by the saturation solubility of the cyclodextrin derivative in the buffer which, in the case of hydroxyethyl / 3-cyclodextrin (MS 0.43), is reached at 7.2 g / ml. 100 ml.

Ved sammenligning af f.eks. resultaterne opnået med indometacin med de, der er anført i tysk offentliggørelsesskrift 31 18 218 for 2,6-di-0-methyl-/5-cyclodextrin (fig. 2) vil det ses, at hydroxyethylderivatet har en betydeligt højere kompleksdannelseskonstant 30 (sammenlign de forskellige hældninger på fig. 1 og 2).When comparing e.g. the results obtained with indomethacin with those disclosed in German disclosure 31 18 218 for 2,6-di-0-methyl-5-cyclodextrin (Fig. 2), it will be seen that the hydroxyethyl derivative has a significantly higher complex formation constant 30 (compare the different slopes of Figures 1 and 2).

I DK 175288 B1 II DK 175288 B1 I

I s II s I

I Eksempel 2 IIn Example 2 I

I A. Mætningsopløseligheden ved 25°C af forskellige lægemidler blev bestemt under an- IIn A. The saturation solubility at 25 ° C of various drugs was determined under I

I vendelse af en 10% hydroxypropyl-j3-cycJodextrinopløsning (MS 0,35) i phosphatstød- ITurning to a 10% hydroxypropyl-β-cyclodextrin solution (MS 0.35) in phosphate buffer I

I 5 pudeopløsning under samme betingelser som i eksempel 1. Mætningsopløselighedeme IIn 5 cushion solution under the same conditions as in Example 1. The saturation solubilities I

I Si i phosphatstødpudeopløsning og S2 i phosphatstødpudeopløsning og 10% tilsat hy- II Si in phosphate buffer solution and S2 in phosphate buffer solution and 10% added hy-I

I droxypropyl-Ø-cyclodextrin er anført i tabel 1. IThe droxypropyl-β-cyclodextrin is listed in Table 1. I

I Tabel 1 IIn Table 1 I

I 10 II 10 I

I Lægemidler S) (ng/ml) S2(mg/ml) Forhold S):S2 IIn Drugs S) (ng / ml) S2 (mg / ml) Ratio S): S2 I

I Indometacin 0,19 5,72 1: 30,1 IIn Indomethacin 0.19 5.72 1: 30.1 I

I Digitoxin 0,002 1,685 1: 842,5 II Digitoxin 0.002 1.685 1: 842.5 I

I Progesteron 0,0071 7,69 1: 1083,0 II Progesterone 0.0071 7.69 1: 1083.0 I

I 15 Dexamethason 0,083 14,28 1: 172,0 II Dexamethasone 0.083 14.28 1: 172.0 I

I Hydrocortison 0,36 21,58 1: 59,9 II Hydrocortisone 0.36 21.58 1: 59.9 I

I Diazepam 0,032 0,94 1: 29,4 IIn Diazepam 0.032 0.94 1: 29.4 I

I R Opløseligheden af lægemidler i en 40% vandig opløsning af hydroxypropyl-methyl- II R The solubility of drugs in a 40% aqueous solution of hydroxypropyl methyl I

I 20 j3-cyclodextrin (DS 0,96; MS 0,43) blev bestemt på lignende måde. De opnåede resulta- I20 µl cyclodextrin (DS 0.96; MS 0.43) was similarly determined. The results obtained I

I ter er opsummeret i følgende tabel 2, hvori forholdet R mellem mætningsopløselighe- IIter is summarized in the following Table 2, in which the ratio R of saturation solubility I

I den i vand eller ved den anførte pH-værdi med og uden tilsætning af jS-cyclodextrinde- IIn the water or at the indicated pH with and without the addition of β-cyclodextrin I

I rivat er anført for hvert lægemiddel. Opløsningerne fremstillet ifølge opfindelsen viste IThe derivative is listed for each drug. The solutions prepared according to the invention showed I

I sig endvidere at være betydeligt mere stabile sammenlignet med vandige opløsninger. IIn addition, being significantly more stable compared to aqueous solutions. IN

I 25 II 25 I

I 30 II 30 I

9 DK 175288 B19 DK 175288 B1

Tabel 2Table 2

Lægemiddel_ RDrug_R

Itraconazol ved pH 5 96 5 ved pH 2,5 75Itraconazole at pH 5 96 5 at pH 2.5 75

Flunarizin 18Flunarizin 18

Levocabastin ved pH 9,5 81 ved pH 7,4 8Levocabastine at pH 9.5 81 at pH 7.4 8

Ketoconazol 85 10 Flubendazol 39Ketoconazole 85 10 Flubendazole 39

Tubulazol 43Tubulazole 43

Cisaprid 3Cisapride 3

Loperamid 62Loperamide 62

Etomidat 8,5 15 Cinnarizin ved pH 5 28 ved pH 3 12Etomidate 8.5 Cinnarizine at pH 5 28 at pH 3 12

Eksempel 3Example 3

20 I 10 ml phosphatstødpudeopløsning blev opløst 0,7 g hydroxyethyl-/?-cyclodextrin (MS 0,43) sammen med 0,04 g indometacin ved 25°C, indtil der var dannet en klar opløsning. Denne opløsning blev filtreret gennem et membranfilter (0,22 micron) og under laminar strømning fyldt i en forud steriliseret injektionsflaske, der blev lagret ved 21°CIn 10 ml of phosphate buffer solution was dissolved 0.7 g of hydroxyethyl - / - cyclodextrin (MS 0.43) together with 0.04 g of indomethacin at 25 ° C until a clear solution was formed. This solution was filtered through a membrane filter (0.22 micron) and loaded under a laminar flow into a pre-sterilized vial stored at 21 ° C.

(B). Ved en parallel prøve blev en mættet indometacinopløsning i en phosphatstødpu-25 deopløsning (0,21 mg pr. ml) lagret under samme betingelser (A). Lægemiddelkoncen-trationeme bestemt ved højtryksvæskekromatografi er anført tabel 3. Den meget forbedrede stabilitet af midlet ifølge opfindelsen fremgår klart.(B). In a parallel sample, a saturated indomethacin solution in a phosphate buffer solution (0.21 mg per ml) was stored under the same conditions (A). The drug concentrations determined by high pressure liquid chromatography are given in Table 3. The much improved stability of the agent according to the invention is clearly evident.

3030

I DK 175288 B1 II DK 175288 B1 I

I 10 II 10 I

I Tabel 3 IIn Table 3 I

I Lagringstid i uger Indometacinindhold (%) IShelf life in weeks Indomethacin content (%) I

I _A_B II _A_B I

I 5 0 100,1 99,7 ' II 100 100.1 99.7 'I

I 2 91,2 99,9 . II 2 91.2 99.9. IN

I 4 79,1 98,1 II 4 79.1 98.1 I

I 6 69,8 98,6 II 6 69.8 98.6 I

I 8 64,8 98,4 II 8 64.8 98.4 I

I 10 II 10 I

I Eksempel 4 (injicerbart præparat) IIn Example 4 (injectable preparation) I

I 0,35 g hydroxypropyl-/3-cyclodextrin (MS 0,35) blev opløst i 5 ml fysiologisk natrium- IIn 0.35 g of hydroxypropyl / 3-cyclodextrin (MS 0.35) was dissolved in 5 ml of physiological sodium I

I chloridopløsning og opvarmet til ca. 35°C, hvorefter der blev tilsat 3 mg diazepam. Ef- IIn chloride solution and heated to approx. 35 ° C, then 3 mg of diazepam was added. Ef- I

I 15 ter lagring i kort tid fremkom en klar opløsning, der blev fyldt i en ampul efter filtre- IFor 15 h of storage for a short time, a clear solution was obtained which was filled into a vial after filtering.

I ring gennem et membranfilter (0,045 micron). IIn the ring through a membrane filter (0.045 micron). IN

I Eksempel 5 (tablet) IIn Example 5 (tablet) I

I 20 I 100 ml vand blev opløst 7 g.hydroxyethyl-/3-cyclodextrin (MS 0,43) og 0,5 g medro- IDissolve 7 g of hydroxyethyl / 3-cyclodextrin (MS 0.43) and 0.5 g of medium in 20 liters of water.

I xyprogesteronacetat. Vandet blev så fordampet i en roterende fordamper. Remanensen IIn xyprogesterone acetate. The water was then evaporated in a rotary evaporator. The residue I

I (75 mg) blev pulveriseret og efter tilsætning af 366‘ mg calciumhydrogenphosphat, II (75 mg) was pulverized and after addition of 366 µg calcium hydrogen phosphate, I

I 2H20, 60 mg majsstivelse, 120 mg cellulosepulver (mikrokrystallinsk), 4,2 mg højdis- IIn 2H 2 O, 60 mg corn starch, 120 mg cellulose powder (microcrystalline), 4.2 mg high

I pers siliciumdioxid (AEROSIL®200) og 4,8 g magniumstearat, blev der fremstillet tab- IIn purple silica (AEROSIL®200) and 4.8 g of magnesium stearate, tabs were prepared.

I 25 letter med en vægt på 630,0 mg og omfattende 5 mg lægemiddel pr. enhedsdosis. Op- II 25 facilitates with a weight of 630.0 mg and comprising 5 mg of drug per day. unit dose. Up in

I løsningshastigheden af medroxyprogesteronacetatet af dette præparat er 21 gange høje- IAt the dissolution rate of the medroxyprogesterone acetate of this preparation is 21 times higher

I re end af en tablet omfattende samme indifferente bestanddele uden tilsætning af β-cyc- IIn re of a tablet comprising the same inert ingredients without the addition of β-cycl I

I lodextrinetheren. IIn the lodextrin ether. IN

I 30 II 30 I

11 DK 175288 B111 DK 175288 B1

Eksempel 6 55 g hydroxyethyl-/3-cyclodextrin (MS 0,43) og 14 mg vitamin A-acetat blev opløst under omrøring i 100 ml vand eller sukkeropløsning (5% vandig opløsning) i løbet af 5 2,5 time under en nitrogenatmosfære. Efter filtrering gennem et membranfilter (0,45 micron) blev opløsningen fyldt i ampuller og steriliseret eller fyldt i dryppeflasker med tilsætning af 0,4% chlorbutanol som konserveringsmiddel.Example 6 55 g of hydroxyethyl / 3-cyclodextrin (MS 0.43) and 14 mg of vitamin A acetate were dissolved with stirring in 100 ml of water or sugar solution (5% aqueous solution) over 2.5 hours under a nitrogen atmosphere. . After filtration through a membrane filter (0.45 micron), the solution was filled into ampoules and sterilized or filled in drip bottles with the addition of 0.4% chlorobutanol as a preservative.

Eksempel 7 10 5 eller 7,5 g hydroxyethyl-/3-cyclodextrin (MS 0,43) og 0,5 eller 0,75 g lidocain blev opløst i 100 ml fysiologisk natriumchloridopløsning ved 30°C (B). Injektionsopløsninger, Øjendråbevæsker og opløsninger til topisk anvendelse blev fremstillet deraf som beskrevet i eksempel 6. Ved sammenligning af den anæstetiske virkning af disse opløs-.Example 7 10 5 or 7.5 g of hydroxyethyl / 3-cyclodextrin (MS 0.43) and 0.5 or 0.75 g of lidocaine were dissolved in 100 ml of physiological sodium chloride solution at 30 ° C (B). Injection solutions, eye drops and topical solutions were prepared therefrom as described in Example 6. By comparing the anesthetic effect of these solutions.

15 ninger i dyreforsøg med en vandig lidocain HC1 opløsning (A) iagttages en forlængelse af varigheden af virkningen med 300%. Prøve: rotter, injektion af 0,1 ml i haleroden i nærheden af de højre eller venstre nervefillamenter og elektrisk irritation. Forsøgsresultaterne er opsummeret i tabel 4.In animal experiments with an aqueous lidocaine HCl solution (A), an extension of the duration of action was observed by 300%. Sample: rats, 0.1 ml injection into the tail root near the right or left nerve filaments and electrical irritation. The experimental results are summarized in Table 4.

20 Tabel 4 Lægemiddelkoncentration Varighed af virkning (min) Forlængelse (%)_A_B_(%} 0,5 56 163 291 25 0,75 118 390 33020 Table 4 Drug concentration Duration of action (min) Extension (%) _ A_B _ (%} 0.5 56 163 291 25 0.75 118 390 330

Eksempel 8 6 mg dexamethason og 100 mg hydroxyethyl-Ø-cyclodextrin (MS 0,43) blev opløst i 5 30 ml vand, steriliseret ved filtrering gennem et membranfilter (0,22 micron) og pakket i en aerosolbeholder, der gør det muligt at dispensere 0,1 ml pr. dosis.Example 8 6 mg of dexamethasone and 100 mg of hydroxyethyl-E-cyclodextrin (MS 0.43) were dissolved in 5 ml of water, sterilized by filtration through a membrane filter (0.22 micron) and packed in an aerosol container allowing dispense 0.1 ml per dosage.

--- -----:- ——--- -----: - ——

I DK 175288 B1 II DK 175288 B1 I

I 12 II 12 I

I Eksempel 9 IIn Example 9 I

I Den akutte intravenøse toxicitet af nogle jS-cyclodextriner blev afprøvet på rotter med IThe acute intravenous toxicity of some β-cyclodextrins was tested in rats with I

I følgende resultater. Det viste sig overraskende, at toxiciteten af derivaterne, der anven- IIn the following results. Surprisingly, it was found that the toxicity of the derivatives used

I 5 des ifølge opfindelsen, er en hel størrelsesorden lavere. IBy December 5 according to the invention, an entire order of magnitude is lower. IN

I Tabel 5 IIn Table 5 I

I LP™ i rotter (i.v.l i mg/kg leeemsvægt IIn LP ™ in rats (i.v.l in mg / kg body weight I

I 10 II 10 I

I /3-cyclodextrin 453 II / 3-cyclodextrin 453 I

I Dimethyl-/3-cyclodextrin (DS 2,0) 200-207 II Dimethyl / 3-cyclodextrin (DS 2.0) 200-207 I

I Hydroxypropyl-methyl-Ø-cyclodextrin >2000* IIn Hydroxypropyl-methyl-E-cyclodextrin> 2000 * I

I (DS 0,96; MS 0,43) ( II (DS 0.96; MS 0.43) (I

I 15 II 15 I

I * en højere dosis er ikke blevet afprøvet. I mus var værdien > end 4000 mg/kg.In * a higher dose has not been tested. In mice, the value was> than 4000 mg / kg.

I Den hæmolytiske virkning af methyletheren ifølge tysk offentliggørelsesskrift 31 18 II The hemolytic effect of the methyl ether according to German publication 31 31 I

I 218 blev sammenlignet med virkningen af en ether anvendt ifølge opfindelsen. Til dette IIn 218 was compared with the effect of an ether used according to the invention. For this I

I 20 formål blev 100 μΐ af en fysiologisk natriumchloridopløsning med et cyclodextrinind- IFor 20 purposes, 100 μΐ of a physiological sodium chloride solution with a cyclodextrin indi-

I hold på 10%, 800 μΐ af en stødpude (400 mg MOPS, 36 mg Na2HP04, 2 H20, 1,6 g IIn hold of 10%, 800 μΐ of a buffer (400 mg MOPS, 36 mg Na2HP04, 2 H2O, 1.6 g I

I NaCl i 200 ml H20) og 100 μΐ af en suspension af humane røde blodceller (tre gange IIn NaCl in 200 ml of H2 O) and 100 μΐ of a suspension of human red blood cells (three times I)

I vasket med natriumchloridopløsning) blandet i 30 minutter ved 37°C. Derefter blevWashed with sodium chloride solution) mixed for 30 minutes at 37 ° C. Then became

I blandingen centrifugeret og den optiske tæthed blev bestemt ved 540 nm. IThe mixture was centrifuged and the optical density determined at 540 nm. IN

I 25 II 25 I

I Kontroller: II Controls: I

I a) 100 μΐ natriumchloridopløsning + stødpude -> 0%hæmolyse I(A) 100 μΐ sodium chloride solution + buffer -> 0% hemolysis I

I b) 900 μΐ vand -* 100%hæmolyse I(B) 900 μΐ water - * 100% hemolysis I

I 30 De opnåede resultater er opsummeret i følgende tabel 6, hvori der er anført de koncen- mI 30 The results obtained are summarized in the following Table 6, which lists the cons

I trationer, ved hvilke der skete 50% og 100% hæmolyse. IIn traces at which 50% and 100% hemolysis occurred. IN

13 DK 175288 B113 DK 175288 B1

Tabel 6Table 6

Stof_c50%_c100%Stof_c50% _c100%

Dimethyl-/5-CD 0,33% 0,5% 5 (DS 2,0)Dimethyl / 5-CD 0.33% 0.5% 5 (DS 2.0)

Methyl-/3-CD 0,53% 0,8% (DS 1,79)Methyl / 3-CD 0.53% 0.8% (DS 1.79)

Hydroxypropyl-methyl-/3-CD 1,5% 4% (DS 0,96; MS 0,43%) 10Hydroxypropyl methyl / 3-CD 1.5% 4% (DS 0.96; MS 0.43%)

Resultaterne viser, at den hæmolytiske virkning af hydroxypropylmethyletheren er ca.The results show that the hemolytic effect of the hydroxypropyl methyl ether is approx.

S til 8 gange svagere end virkningen af den kendte dimethylether. Dyreforsøg har endvidere vist, at hydroxyalkyletheme ikke forårsager irritation af slimhinden og øjnene i modsætning til methyletheme.S to 8 times weaker than the action of the known dimethyl ether. Animal studies have further shown that the hydroxyalkyl ethers do not cause irritation of the mucosa and eyes as opposed to the methyl etheme.

1515

Claims (14)

1. Farmaceutisk middel indeholdende inklusionsforbindelser af lægemidler, der er I I 5 ustabile eller sparsomt opløselige i vand, med en cyclodextrin, kendetegnet ved, at I I cyclodextrinen er delvist forethret β-cyclodextrin, hvis ethersubstituenter er hydroxy- I I ethyl-, hydroxypropyl- eller dihydroxypropylgrupper og en del af ethersubstituenteme I I valgfrit kan være methyl- eller ethylgrupper, og den foretherede /3-cyclodextrin har en I I vandopløselighed på mere end 1,8 g i 100 ml vand, idet inklusionsforbindelser af reti- I I 10 noider med /3-cyclodextriner i det omfang, at deres ethersubstituenter er methyl-, ethyl- I I eller 2-hydroxyethylgrupper, såvel som inklusionsforbindelser af lægemidler, som er I I sparsomt vandopløselige eller ustabile i vand, med blandinger af /5-cyclodextrinepi- I I chlorhydrinderivater, som har en middel-molekylvægt på (Mw) 5300, er udelukket. I I 15Pharmaceutical agent containing inclusion compounds of drugs which are unstable or sparingly soluble in water, with a cyclodextrin, characterized in that the and a portion of the ether substituents II may optionally be methyl or ethyl groups, and the etherated / 3-cyclodextrin has a II water solubility of more than 1.8 g in 100 ml of water, inclusion compounds of retinoids with / 3-cyclodextrins in to the extent that their ether substituents are methyl, ethyl II or 2-hydroxyethyl groups, as well as inclusion compounds of drugs which are II sparingly water-soluble or unstable in water, with mixtures of / 5-cyclodextrinepi-II chlorohydrin derivatives having an intermediate molecular weight of (Mw) 5300, is excluded. I I 15 2. Middel ifølge krav 1, kendetegnet ved, at den delvis forethrede β-cyclodextrin har I I en molær substitutionsgrad for hydroxyalkylgrupper på 0,2 til 10 og en substitutions- I I grad for alkylgrupper på 0,2 til 2,0. IAgent according to claim 1, characterized in that the partially etherated β-cyclodextrin has an I molar degree of substitution for hydroxyalkyl groups of 0.2 to 10 and a degree of substitution for alkyl groups of 0.2 to 2.0. IN 3. Middel ifølge krav 1 eller 2, kendetegnet ved, at det omfatter lægemiddel og β- I I 20 cyclodextrinethere i et molært forhold på 1:6 til 4:1. IAn agent according to claim 1 or 2, characterized in that it comprises drug and β-I to 20 cyclodextrin ethers in a molar ratio of 1: 6 to 4: 1. IN 4. Middel ifølge krav 1 til 3, kendetegnet ved, at det som lægemiddel indeholder et I I ikke-steroidt antirheumatisk middel, et steroid, et hjerteglycosid eller derivater afben- I I zodiazepin, benzimidazol, piperidin, piperazin, imidazol eller triazol. I I 25 IAn agent according to claims 1 to 3, characterized in that it contains as a drug an I I non-steroidal anti-rheumatic agent, a steroid, a cardiac glycoside or derivatives of benz I, ziaziazepine, benzimidazole, piperidine, piperazine, imidazole or triazole. I I 25 I 5. Middel ifølge ethvert af kravene 1 til 4, kendetegnet ved, at det som lægemiddel I I indeholder etomidat. IAn agent according to any one of claims 1 to 4, characterized in that it contains, as a drug 11, etomidate. IN 6. Middel ifølge ethvert af kravene 1 til 4, kendetegnet ved, at det som lægemiddel I I 30 indeholder ketoconazol. I DK 175288 B1An agent according to any one of claims 1 to 4, characterized in that it contains as ketoconazole as a medicament I 30. In DK 175288 B1 7. Middel ifølge ethvert af kravene 1 til 4, kendetegnet ved, at det som lægemiddel indeholder itraconazol.An agent according to any one of claims 1 to 4, characterized in that it contains as itraconazole as a medicament. 8. Middel ifølge ethvert af kravene 1 til 4, kendetegnet ved, at det som lægemiddel « 5 indeholder levocabastin.An agent according to any one of claims 1 to 4, characterized in that, as a medicament '5, it contains levocabastine. 9. Middel ifølge ethvert af kravene 1 til 4, kendetegnet ved, at det som lægemiddel indeholder flunarizin.An agent according to any one of claims 1 to 4, characterized in that it contains as a drug flunarizine. 10. Middel ifølge ethvert af kravene 1 til 4, kendetegnet ved, at der som lægemiddel indeholder tubulazol.An agent according to any one of claims 1 to 4, characterized in that it contains as a drug tubulazole. 11. Fremgangsmåde til fremstilling af et farmaceutisk middel ifølge ethvert af kravene 1 til 10, kendetegnet ved, at /3-cyclodextrinetheren opløses i vand, og det valgte læge- 15 middel derefter tilsættes, hvorpå opløsningen af inklusionsforbindelsen, der derved fås, eventuelt tørres under anvendelse af i og for sig kendte måder.Process for the preparation of a pharmaceutical according to any one of claims 1 to 10, characterized in that the β-cyclodextrin ether is dissolved in water and the selected drug is then added, whereupon the solution of the inclusion compound thus obtained is optionally dried. using methods known per se. 12. Fremgangsmåde ifølge krav 11, kendetegnet ved, at den efter fjernelse af opløsningsmidlet opnåede rest pulveriseres og eventuelt efter tilsætning af yderligere hjæl- 20 pestoffer omdannes til en fast administrerbar form.Process according to claim 11, characterized in that the residue obtained after removal of the solvent is pulverized and, optionally, after addition of additional excipients, is converted into a solid, administrable form. 13. Fremgangsmåde ifølge krav 11 eller krav 12, kendetegnet ved, at yderligere fysiologisk forligelige stoffer sættes til vandet. 1 30Process according to claim 11 or claim 12, characterized in that additional physiologically compatible substances are added to the water. 1 30 14. Fremgangsmåde ifølge krav 13, kendetegnet ved, at natriumchlorid, glucose, mannitol, sorbitol, xylitol eller en phosphat- eller citratstødpude sættes til vandet.Process according to claim 13, characterized in that sodium chloride, glucose, mannitol, sorbitol, xylitol or a phosphate or citrate buffer are added to the water.
DK198503595A 1983-12-21 1985-08-07 Pharmaceutical agents containing drugs which are unstable or sparingly soluble in water, and methods for their preparation DK175288B1 (en)

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PCT/EP1984/000417 WO1985002767A1 (en) 1983-12-21 1984-12-20 Pharmaceutical compositions containing drugs which are instable or sparingly soluble in water and methods for their preparation
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DE3481680D1 (en) 1990-04-26
EP0149197A3 (en) 1985-08-14
EP0149197B1 (en) 1990-03-21
JPS61500788A (en) 1986-04-24
JPH0570612B2 (en) 1993-10-05
CA1222697A (en) 1987-06-09
FI853198A0 (en) 1985-08-20
DE3346123A1 (en) 1985-06-27
WO1985002767A1 (en) 1985-07-04
ATE51145T1 (en) 1990-04-15
FI853198L (en) 1985-08-20
FI86140B (en) 1992-04-15
HK131293A (en) 1993-12-03
NO2000007I1 (en) 2000-09-21
NL980009I1 (en) 1998-05-06
HUT40561A (en) 1987-01-28
DK359585A (en) 1985-08-07
EP0149197A2 (en) 1985-07-24
AU3835285A (en) 1985-07-12
ZA8410042B (en) 1985-09-25
DK359585D0 (en) 1985-08-07
EP0149197B2 (en) 1997-01-08
LU90283I2 (en) 1998-11-03
AU565966B2 (en) 1987-10-01
SG24893G (en) 1993-08-06
HU200943B (en) 1990-09-28
FI86140C (en) 1992-07-27
CY1689A (en) 1994-01-14

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