SI9300006A - Process for the preparation of substituted steroidal derivatives - Google Patents

Process for the preparation of substituted steroidal derivatives Download PDF

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SI9300006A
SI9300006A SI19939300006A SI9300006A SI9300006A SI 9300006 A SI9300006 A SI 9300006A SI 19939300006 A SI19939300006 A SI 19939300006A SI 9300006 A SI9300006 A SI 9300006A SI 9300006 A SI9300006 A SI 9300006A
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reagent
process according
halogen
chloride
source
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Neil Howard Baine
Donald Nathaniel Kline
Richard Eric Mewshaw
Franklin Owings
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Smithkline Beecham Corporation
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    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07JSTEROIDS
    • C07J9/00Normal steroids containing carbon, hydrogen, halogen or oxygen substituted in position 17 beta by a chain of more than two carbon atoms, e.g. cholane, cholestane, coprostane
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07JSTEROIDS
    • C07J43/00Normal steroids having a nitrogen-containing hetero ring spiro-condensed or not condensed with the cyclopenta(a)hydrophenanthrene skeleton
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07JSTEROIDS
    • C07J3/00Normal steroids containing carbon, hydrogen, halogen or oxygen, substituted in position 17 beta by one carbon atom
    • C07J3/005Normal steroids containing carbon, hydrogen, halogen or oxygen, substituted in position 17 beta by one carbon atom the carbon atom being part of a carboxylic function
    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07JSTEROIDS
    • C07J41/00Normal steroids containing one or more nitrogen atoms not belonging to a hetero ring
    • C07J41/0033Normal steroids containing one or more nitrogen atoms not belonging to a hetero ring not covered by C07J41/0005
    • C07J41/0066Normal steroids containing one or more nitrogen atoms not belonging to a hetero ring not covered by C07J41/0005 the 17-beta position being substituted by a carbon atom forming part of an amide group

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  • Chemical & Material Sciences (AREA)
  • Organic Chemistry (AREA)
  • Health & Medical Sciences (AREA)
  • General Health & Medical Sciences (AREA)
  • Steroid Compounds (AREA)
  • Organic Low-Molecular-Weight Compounds And Preparation Thereof (AREA)
  • Nitrogen Condensed Heterocyclic Rings (AREA)

Abstract

The invention provides an improved process for the preparation of a halogenated steroidal diene. The process involves the simultaneous transformation of the steroidal 3-one to 3-halo and 17-carboxylic acid to 17-carboxamide in a single reaction without the isolation of an intermediate. The process takes place by reacting the steroidal starting material with a halogen-Vilsmeier reagent.

Description

SMITHKLINE BEECHAM CORPORATIONSMITHKLINE BEECHAM CORPORATION

Postopek za pripravo substituiranih steroidnih derivatovA process for the preparation of substituted steroid derivatives

Področje izumaFIELD OF THE INVENTION

Predloženi izum se nanaša na izboljšan postopek za pripravo substituiranih steroidnih dienov. Takšne spojine so opisali v US patentu št. 5,017,568, izdanem 21. maja 1991, Holt et al., kot uporabne pri inhibiciji steroida 5-a-reduktaze.The present invention relates to an improved process for the preparation of substituted steroid dienes. Such compounds have been described in U.S. Pat. No. 5,017,568, issued May 21, 1991, by Holt et al., As useful in inhibiting 5-α-reductase steroid.

Ozadje izumaBACKGROUND OF THE INVENTION

Postopki za pripravo substituiranih steroidnih dienskih derivatov so bili že opisani. V US patentu št. 5,017,568 so poročali posebno o uporabi oksalil bromida za pretvorbo steroidnih a,/3-nenasičenih-3-ketonov v 3-bromo-3,5-dienske intermediate (v 40 % dobitku), ki ji sledi katalitična ali z alkilitijem posredovana karboksilacija (v 15 % dobitku, ko so uporabili N-butil litij), da so dobili steroidne derivate 3,5-dien-3karboksilne kisline.Methods for the preparation of substituted steroidal diene derivatives have already been described. In U.S. Pat. 5,017,568 specifically reported the use of oxalyl bromide for the conversion of steroidal α, 3-unsaturated-3-ketones into 3-bromo-3,5-diene intermediates (in 40% yield), followed by catalytic or alkylityl-mediated carboxylation (in 15% yield when using N-butyl lithium) to give the steroid derivatives of 3,5-diene-3-carboxylic acid.

Razen nizkega celokupnega dobitka, je dodatna pomanjkljivost te objave ta, da je oksalil bromid strupena, draga tekočina, ki jo težko skladiščimo in ni zlahka razpoložljiva v večjih količinah, potrebnih za industrijski postopek.Aside from the low overall yield, an additional disadvantage of this publication is that oxalyl bromide is a toxic, expensive liquid that is difficult to store and is not readily available in large quantities required for the industrial process.

Uporaba oksalil klorida za halogeniranje steroidnih α,/3-nenasičenih ketonov v kloro-steroidne diene uspeva z le majhnimi rezultati. Nadalje relativno nizka reaktivnost nastalega kloro substituenta poseduje ne-trivialne sintezne težnje v kasnejših transformacijah. Tako v stroki obstaja potreba po varnem, ekonomičnem in zanesljivem postopku za halogeniranje steroidnih ajS-nenasičenih ketonov v halo1,3-diene. Prenostno z omenjeno metodo bromiramo ali jodiramo sterodne αβnenasičene ketone v njihove ustrezne halo-l,3-diene.The use of oxalyl chloride to halogenate steroidal α, β-unsaturated ketones into chloro-steroidal dienes succeeds with only limited results. Furthermore, the relatively low reactivity of the resulting chloro substituent possesses non-trivial synthesis tendencies in later transformations. Thus, there is a need in the art for a safe, economical and reliable process for halogenating steroid aiS-unsaturated ketones into halo 1,3-dienes. Preferably, by said method, the brominated or iodinated α-unsaturated ketones are brominated or iodinated into their corresponding halo-1,3-dienes.

Povezetek izumaSummary of the Invention

Predloženi izum se nanaša na postopek za halogeniranje spojine z mnogovrstnimi funkcionalnimi skupinami na isti molekuli.The present invention relates to a process for halogenating a compound with multiple functional groups on the same molecule.

Predloženi izum se nanaša na izboljšan postopek za pretvorbo steroidnih αβnansičenih ketonov v njihove ustrezne halo-l,3-dienske derivate.The present invention relates to an improved process for the conversion of steroidal αβ-unsaturated ketones into their corresponding halo-1,3-diene derivatives.

Predloženi izum se nanaša na izboljšan postopek za formiranje kislinskega halida iz substituenta steroidne karboksilne kisline, ki mu sledi nukleofilna zamenjavo omenjenega halida.The present invention relates to an improved process for the formation of an acid halide from a steroid carboxylic acid substituent followed by nucleophilic replacement of said halide.

Predloženi izum s natančneje nanaša na izboljšan postopek za in situ pretvobo steroidnih karboksilnih kislin v steroidne karboksamide.The present invention more specifically relates to an improved process for the in situ conversion of steroid carboxylic acids into steroid carboxamides.

Predloženi izum se natančneje nanaša na postopek za simultano bromiranje in amidacijo steroidnih spojin 3-on-4-en-17-karboksilne kisline.The present invention relates more specifically to a process for the simultaneous bromination and amidation of 3-on-4-en-17-carboxylic acid steroid compounds.

Predloženi izum se natančneje nanaša na izboljšan postopek za pripravo N-t-butilandrost-3,5-dien-17/3-karboksamid-3-karboksilne kisline.The present invention more specifically relates to an improved process for the preparation of N-t-butylandrost-3,5-diene-17/3-carboxamide-3-carboxylic acid.

Podobnejši opis izumaA more similar description of the invention

Pojem simultana, kot ga uporabljamo tukaj pomeni, da izvedemo transformacijo steroidnega 3-ona v 3-halo in 17-karboksilne kisline v 17-karboksamid z eno reakcijo brez izolacije intermediata.The term simultaneous, as used herein, means the transformation of steroid 3-one into 3-halo and 17-carboxylic acids into 17-carboxamide in a single reaction without isolation of the intermediate.

Kot smo uporabili zgoraj in po vsem nadaljnem opisu in zahtevkih, ogljike steroidnega jedra oštevilčimo in obroče označimo s črkami, kot sledi:As used above and after all the further descriptions and claims, the carbon of the steroid core is numbered and the rings are numbered as follows:

Pojem znižana temperatura, kot ga uporabljamo tukaj, pomeni pod 25°C, prednostno med -15 in 15°C, najbolj prednostno med 0 in 10°C.The term "reduced temperature" as used herein means below 25 ° C, preferably between -15 and 15 ° C, most preferably between 0 and 10 ° C.

Pojem pripajalni reagent, kot ga uporabljamo tukaj, pomeni spojino in/ali pogoje, ki so sposobni presnovitve z metaliranim delom, da formiramo kisliski, esterski, alkilkarbonilni ali C120 alkilni del. Prednostno je omenjeni metalirani del, z litijem metaliran del, pripravljen s presnovo ustreznega halogeniranega dela z alkillitijevim reagentom. Spojine uporabne kot pripajalni reagenti vključujejo kloro formate, alkil bromide in kislinske kloride. Prednostno v omenjenem pripajalnem reagentu uporabimo ogljikov dioksid kot reakcijsko spojino.The term coupling reagent as used herein means a compound and / or conditions that are capable of being metabolised by a metallic moiety to form an acidic, ester, alkylcarbonyl or C 120 alkyl moiety. Preferably, said metallic moiety, a lithium metal moiety, is prepared by metabolizing the corresponding halogenated moiety with an alkylity reagent. Compounds useful as coupling reagents include chloro formates, alkyl bromides, and acid chlorides. Preferably carbon dioxide is used as the reaction compound in said coupling reagent.

Pojem kislina, kot ga uporabljamo tukaj, pomeni katerokoli skupino, ki je sposobna reagirati kot protonski donor, vključno vendar ne omejeno z; -COOH, -P(O)(0H)2, PH((O)OH, -SO3H in -(CH^-COOH.The term acid as used herein means any group capable of reacting as a proton donor, including but not limited to; -COOH, -P (O) (0H) 2 , PH ((O) OH, -SO 3 H and - (CH 2 -COOH.

Pojem ester, kot ga uporabljamo tukaj, pomeni skupino, ki sestoji iz kisline, kot je definirano zgoraj, v kateri je donorski proton ali protoni zamenjan z alkilnimi substituenti.The term ester as used herein means a group consisting of an acid, as defined above, in which the donor proton or protons are replaced by alkyl substituents.

Pojem topilo ali primerno topilo, kot ga uporabljamo tukaj, pomeni organsko topilo, kot je merilen klorid, etilen klorid, kloroform, ogljikov tetraklorid, tetrahidrofuran (THF), etil eter ogljik, toluen ali etil acetat.The term solvent or suitable solvent as used herein means an organic solvent such as measuring chloride, ethylene chloride, chloroform, carbon tetrachloride, tetrahydrofuran (THF), ethyl ether carbon, toluene or ethyl acetate.

Pojem halogen-Vilsmeierjev reagent, kot ga uporabljamo tukaj, pomeni halogenirani disubstituirani formamidni reagent s strukturo:The term halogen-Wilsmeier reagent as used herein means a halogenated disubstituted formamide reagent having the structure:

χθγχθγ

N=C v kateri R5 in R6 neodvisno izberemo izmed alkilne, arilne ali arilalkilne skupine; in je X Br ali J; in je Y proti-ion, ki ga pripravimo s:N = C in which R 5 and R 6 are independently selected from an alkyl, aryl or arylalkyl group; and X is Br or J; and Y is the counter ion prepared by:

a) presnovitvijo, prednostno pri znižanih temperaturah, kloridnega vira, kot je oksalil klorid ali tionil klorid, z disubstituiranim formamidnim reagentom, kot je dialkil substituiran formamidni reagent, prednostno dimetilformamid, v primernem topilu, prednostno metilen kloridu, da dobimo kloro-Vilsmeierjev reagent, omenjeni kloroVilsmeierjev reagent presnovimo in situ, prednostno pri znižanih temperaturah, z virom broma ali virom joda, prednostno plinskim bromovodikom alia) metabolism, preferably at reduced temperatures, of a chloride source, such as oxalyl chloride or thionyl chloride, with a disubstituted formamide reagent such as dialkyl substituted formamide reagent, preferably dimethylformamide, in a suitable solvent, preferably methylene chloride, to obtain chloro chloride, said chloroVilsmeier reagent is reacted in situ, preferably at reduced temperatures, with a bromine source or iodine source, preferably a gas hydrobromide, or

b) presnovitvijo, prednostno pri znižanih temperaturah, bromidnega vira ali jodidnega vira, prenostno oksalil bromida, z disubstituiranim formamidnim reagentom, kot je dialkil substituirani formamidni reagent, prednostno dimetilformamid v primernem topilu, prednostno metilen kloridu.b) metabolizing, preferably at reduced temperatures, a bromide source or an iodide source, preferably oxalyl bromide, with a disubstituted formamide reagent such as a dialkyl substituted formamide reagent, preferably dimethylformamide in a suitable solvent, preferably methylene chloride.

Predloženi izum se torej nanaša na in situ pripravo in uporabo bromoVilsmeierjevega reagenta ali jodo-Vilsmeierjevega reagenta, pri čemer reagenta pripravimo varno in ekonomično iz znanih in zlahka dostopnih reagentov, prednostno ustreznega kloro-Vilsemierjevega reagenta. Kot tak ima predloženi izum uporabnost v vseh reakcijah, kjer uporabimo bromo-Vilsmeierjeve reagente ali jodo-Vilsmeierjeve reagente.The present invention therefore relates to the in situ preparation and use of a bromoVilsmeier reagent or an iodo-Vilsmeier reagent, wherein the reagent is prepared safely and economically from known and readily available reagents, preferably a suitable chloro-Vilsemier reagent. As such, the present invention has utility in all reactions where bromo-Vilsmeier reagents or iodo-Vilsmeier reagents are used.

Prednostni alkillitijevi reagenti za uporabo tukaj, vključujejo n-butillitij, sek-butillitii in terc-butillitii.Preferred alkyllithium reagents for use herein include n-butyllithium, sec-butyllithium and tert-butyllithium.

Če ni določeno drugače, pojem halogen in njegovi derivati, kot ga uporabljamo tukaj, pomeni brom ali jod.Unless otherwise specified, the term halogen and its derivatives as used herein means bromine or iodine.

Farmacevtsko sprejemljive soli, hidrati in solvati spojin s formulo (I) pripravimo, kjer je primerno, s postopki dobro znanimi strokovnjakom.Pharmaceutically acceptable salts, hydrates and solvates of the compounds of formula (I) are prepared, where appropriate, by methods well known in the art.

Predloženi izum se nanaša na postopek za proizvodnjo spojine s formulo (I):The present invention relates to a process for the production of a compound of formula (I):

v kateri:in which:

je R1 NR3R4, kjer R3 in R4 vsakega neodvisno izbreremo izmed vodika, C^alkila, C^cikloalkila, fenila; ali R3 in R4 skupaj z dušikom, na katerega sta vezana, predstravljata 5-6 členski nasičen obroč, ki vsebuje do en drugačen heteroatom izbran izmed kisika in dušika; in je R2 kislina, ester, Cj^alkilkarbonil ali Cj 2Qalkil;R 1 is NR 3 R 4 wherein R 3 and R 4 are each independently selected from hydrogen, C 1-6 alkyl, C 1-4 cycloalkyl, phenyl; or R 3 and R 4 together with the nitrogen to which they are attached represent a 5-6 membered saturated ring containing up to one different heteroatom selected from oxygen and nitrogen; and R 2 is an acid, ester, C 1-6 alkylcarbonyl or C 1-2 alkyl;

ali njene farmacevtsko sprejemljive soli, hidrata ali solvata, ki vključuje presnovitev, pri zmanjšani temperaturi, spojine s formulo (II)or a pharmaceutically acceptable salt, hydrate or solvate thereof, including reduced-metabolism, compounds of formula (II)

(II) v prisotnosti halogen-Vilsmeierjevega reagenta in topila, nato reakcijo ustavimo s presežnim H-R1, kjer je R1, kot je opisano zgoraj, da dobimo spojino s formulo (III):(II) in the presence of a halogen-Vilsmeier reagent and a solvent, the reaction is then stopped with excess HR 1 where R 1 is as described above to give the compound of formula (III):

halogen (III) v kateri je R1, kot je definirano zgoraj, in nato v primernem topilu in pri znižani temperaturi dodamo alkillitijev reagent, kateremu sledi pripajalni reagent, da dobimo spojino s formulo (I), če je R3 in/ali R4 H, spojino s formulo (III) podvržemo bazičnemu mediju, primernemu za selektivno deprotoniranje amida predno dodamo alkillitijev reagent, in nato v danem primeru dobimo njeno farmacevtsko sprejemljivo sol, hidrat ali solvat.halogen (III) in which R 1 is as defined above and then in a suitable solvent and at reduced temperature an alkylityl reagent is added followed by a coupling reagent to give the compound of formula (I) if R 3 and / or R 4 H, the compound of formula (III) is subjected to a basic medium suitable for the selective deprotonation of the amide before the alkylityl reagent is added, and then a pharmaceutically acceptable salt, hydrate or solvate thereof is obtained.

Prednostno omenjeni halogen-Vilsmeierjev reagent pripravimo s spresnovitvijo, prednostno pri znižanih temperaturah, kloridnega vira, kot je oksalil klorid ali tionil klorid, z disubstituiranim formamidnim reagentom, kot je dialkil substituirani formamidni reagent, prednostno dimetilformamidom, v primernem topilu, prenostno metilen kloridu, da dobimo kloro-Vilsmeierjev reagent, pri čemer kloro-Vilsmeierjev reagent presnovimo in situ, prednostno pri znižanih temperaturah, z bromidnim virom ali jodidnim virom, prednostno s plinskim bromovodikom.Preferably, said halogen-Wilsmeier reagent is prepared by, preferably at reduced temperatures, a chloride source such as oxalyl chloride or thionyl chloride, with a disubstituted formamide reagent such as dialkyl substituted formamide reagent, preferably dimethylformamide, in a suitable topidyl, preferably a chloro-Vilsmeier reagent is obtained, whereby the chloro-Vilsmeier reagent is reacted in situ, preferably at reduced temperatures, with a bromide source or an iodide source, preferably with a gas bromine hydrogen.

Kot uporabljamo tukaj, če ni drugače določeno, pomeni Cj nalkil ravno ali razvejano ogljikovodikovo verigo z ogljiki.As used herein, unless otherwise specified, it means a C n alkyl, straight or branched hydrocarbon chain with the carbons.

Kot uporabljamo tukaj, če ni drugače določeno, pomeni alkil ravno ali razvejano ogljikovodikovo verigo.As used herein, unless otherwise specified, alkyl means a straight or branched hydrocarbon chain.

Kot uporabljamo tukaj, če ni drugače določeno, pomeni aril aromatski karbocikličen ali heterocikličen obroč, ki je nesubstituiran ali substituiran z ne-reaktivnimi substituenti.As used herein, unless otherwise specified, an aryl is an aromatic carbocyclic or heterocyclic ring which is unsubstituted or substituted by non-reactive substituents.

Prednostno halogen-Vilsmeierjeve reagente uporabljamo v dihalogenaciji spojin s formulo (II) pripravljamo in uporabljamo in situ.Preferably, the halogen-Vilsmeier reagents used in the dihalogenation of the compounds of formula (II) are prepared and used in situ.

Prednostno je omenjeni halogen-Vilsmeierjev reagent bromo-Vilsmeierjev reagent.Preferably said halogen-Vilsmeier reagent is a bromo-Vilsmeier reagent.

Prednostno je omenjeni bromo-Vilsmeierjev reagent (bromometilen) dimetil amonijev bromid.Preferably said bromo-Wilsmeier reagent is (bromomethylene) dimethyl ammonium bromide.

Prednostne organske kisline, uporabljene, da opišemo R2 v formuli (I), vključujejo: -COOH, -P(O)(OH)2, -PH(O)(OH), -SO3H in -(CH^COOH. Posebno prednostna izmed zgornjih kislin je -COOH.Preferred organic acids used to describe R 2 in formula (I) include: -COOH, -P (O) (OH) 2 , -PH (O) (OH), -SO 3 H, and - (CH ^ COOH Particularly preferred of the above acids is -COOH.

Prednostne baze uporabljene pri pripravi bazičnega medija uporabljenega za selektivno deprotoniranje amida spojin s formulo (II) vključujejo kovinske hidride, alkillitijeve reagente, Grignardove reagente in kovinske alkokside. Prednostne izmed zgoraj opisanih baz so etilmagnezijev bromid, butillitij in etilmagnezijev klorid. Posebno prednostna izmed zgoraj opisanih baz je etilmagnezijev klorid. Prednostno selektivno deprotoniranje omenjenega amida vodimo pri temperaturi nad 25°C, najbolj prednostno med 30 in 50°C.Preferred bases used in the preparation of the basic medium used for the selective deprotonation of the amide of compounds of formula (II) include metal hydrides, alkyllithium reagents, Grignard reagents and metal alkoxides. Preferred bases described above are ethylmagnesium bromide, butyllithium and ethylmagnesium chloride. Particularly preferred of the bases described above is ethylmagnesium chloride. Preferably, the selective deprotonation of said amide is conducted at a temperature above 25 ° C, most preferably between 30 and 50 ° C.

Prednostno je alikl litijev reagent uporabljen, da iniciiramo halogen-kovinsko izmenjavo na spojinah s formulo (III), sek-butillitij.Preferably, an allyl lithium reagent is used to initiate halogen-metal exchange on the compounds of formula (III), sec-butyllithium.

Prednostni vidik predloženega izuma je priprava sterodinih halo-l,3-dienskih sistemov iz sterodinih α,β-nenasičenih ketonov, z uporabo halogen-Vilsmeierjevega reagenta, ki ga pripravimo in uporabimo in situ.An advantageous aspect of the present invention is the preparation of sterodine halo-1,3-diene systems from sterodine α, β-unsaturated ketones using a halogen-Vilsmeier reagent, which is prepared and used in situ.

Prednostni vidik predloženega izuma je s halogen-Vilsmeierjevim reagentom inducirana tvorba kislinskega halidnega dela iz sterodinega karboksilnega kislinskega dela, pri čemer omenjeni kislinski halidni substituent podvržemo premestitvi z nukleofilnim reagentom. Prednostni nukleofilni reagenti, kot jih uporabljamo tukaj, vključujejo H-R1, kjer je R1, kot je definirano zgoraj. Posebno prednosten med zgornjimi nukleofilnimi reagenti je terc-butilamin.An advantageous aspect of the present invention is the formation of an acid halide moiety from the sterodine carboxylic acid moiety by the halogen-Vilsmeier reagent, wherein said acid halide substituent is displaced by the nucleophilic reagent. Preferred nucleophilic reagents as used herein include HR 1 where R 1 is as defined above. Particularly preferred among the above nucleophilic reagents is tert-butylamine.

Prednostno je zato postopek v smislu predloženega izuma posebno uporaben za pripravo spojine s strukturo (ΙΙΙΑ):Preferably, therefore, the process of the present invention is particularly useful for the preparation of a compound of structure (ΙΙΙΑ):

ΟΟ

(ΙΙΙΑ) in pretvorbo le-te v sledečo spojino s strukturo (IA)(ΙΙΙΑ) and its conversion to the following compound of structure (IA)

OOh

IIII

ali njene farmacevtsko sprejemljive soli, hidrata ali solvata.or a pharmaceutically acceptable salt, hydrate or solvate thereof.

Brez nadaljne obdelave verjamemo, da lahko strokovnjah, ob uporabi predhodnega opisa, uporabi predloženi izum do njegovega največjega obsega. Naslednje primere zato razlagamo kot pretežno ponazoritev in ne omejitev obsega predloženega izuma v kateremkoli smislu.Without further elaboration, it is believed that the skilled person, using the foregoing description, can use the present invention to its fullest extent. The following examples are therefore to be construed as predominantly illustrative rather than limiting the scope of the present invention in any sense.

I. Primeri sintezeI. Examples of synthesis

Dimetilformamid, oksalil klorid, oksalil bromid, terc-butilamine, 2,0 M etilmeagnezijev klorid v THF, 1,2 M sek-butillitij v cikloheksanu in (+)-4-holesten-3-on so razpoložlivi pri Aldrich Chemical Co. (Mihvaukee, WI). Plinski bromovodik in plinski ogljikov dioksid sta razpoložljiva pri Matheson (E. Rutherford, NJ). Androst-4-en-3on-17/3-karboksilna kislina je razpoložljiva pri Berlichem, Inc. (Wayne, NJ).Dimethylformamide, oxalyl chloride, oxalyl bromide, tert-butylamines, 2.0 M ethylmagnesium chloride in THF, 1.2 M sec-butyllithium in cyclohexane and (+) - 4-cholesten-3-one are available from Aldrich Chemical Co. (Mihvaukee, WI). Hydrogen bromide gas and carbon dioxide gas are available from Matheson (E. Rutherford, NJ). Androst-4-en-3one-17/3-carboxylic acid is available from Berlichem, Inc. (Wayne, NJ).

3-bromo-androsta-3,5-diene-17/3-karboksilno kislino pripravimo, kot je opisano v U.S. patentu 5,017,568 (Primer 25B (ii)).3-Bromo-androsta-3,5-diene-17/3-carboxylic acid was prepared as described in U.S. Pat. 5,017,568 (Example 25B (ii)).

Primer 1Example 1

17g-i[(l,l-dimetiletil)amino]karbonillandrosta-3,5-dien-3-karboksilna kislina (i) 3-Bromo-N-(l,l-dimetiletil)-androsta-3,5-dien-17/3-karboksamid17g-i [(1,1-dimethylethyl) amino] carbonyl-sulphon-3,5-diene-3-carboxylic acid (i) 3-Bromo-N- (1,1-dimethylethyl) -androsta-3,5-diene 17/3-carboxamide

Bučko pod atmosfero dušika napolnimo s 100 ml metilen klorida in 6,12 ml (2,5 molarnimi ekvivalenti) dimetilformamida. Raztopino ohladimo na 0-5°C, in obdelamo s 6,9 ml (2,5 molarnima ekvivalentoma) oksalil klorida, medtem ko vzdržujemo temeperaturo med 0-10°C. Nastane bela oborina. Po mešanju eno uro,Fill the flask under a nitrogen atmosphere with 100 ml of methylene chloride and 6.12 ml (2.5 molar equivalents) of dimethylformamide. The solution was cooled to 0-5 ° C and treated with 6.9 ml (2.5 molar equivalents) of oxalyl chloride while maintaining the temperature between 0-10 ° C. A white precipitate forms. After stirring for one hour,

50,1 g (19,6 molarnih ekvivalentov) plinskega bromovodika vpihavamo skozi raztopino, medtem ko vzdržujemo temperaturo med 0-10 °C. Suspenzija postane bistra brezbarvna raztopina. Raztopino odplinimo z zmanjšanjem volumna raztopine za okoli eno polovico z vakuumsko destilacijo in vrnemo na prvotni volumen z metilen kloridom. Ta koncentracijski/dopolnilni postopek ponavljamo. Androst-4-en-3-on17/3-karboksilno kislino, 10,0 g (1 molarni ekvivalent), dodamo nastali beli suspenziji in zmes segrejemo na sobno temperaturo in mešamo 2 uri. Reakcijsko zmes prelijemo v posodo, ki vsebuje 100 ml metilen klorida in 23,1 g (10 molarnih ekvivalentov) terc-butilamina, medtem ko vzdržujemo temperaturo med 0-10°C. Zmes mešamo 30 minut. Dodamo okoli 100 ml vode in dvofazno zmes filtriramo skozi blazinico Celita. Organsko fazo ločimo in zmanjšamo na okoli polovico njenega volumna z vakuumsko destilacijo. Raztopino vrnemo na prvotni volumen z acetonom. Ta koncentracijski/dopolnilni postopek ponovimo še dvakrat. Nastalo acetonsko raztopino (okoli 300 ml) segrejemo na okoli 50°C in obdelamo z okoli 100 ml vode, da oborimo produkt. Suspenzijo ohladimo in produkt, 3-bromo-N(l,ldimetiletil)-androsta-3,5-dien-17/3-karboksamid, izoliramo s filtracijo in posušimo. Dobitek 89 %, tal. 181-183°C.50.1 g (19.6 molar equivalents) of the bromine gas are bubbled through the solution while maintaining the temperature between 0-10 ° C. The suspension becomes a clear colorless solution. The solution is degassed by reducing the volume of the solution by about one half by vacuum distillation and returning to its original volume with methylene chloride. We repeat this concentration / replenishment process. Androst-4-en-3-one17 / 3-carboxylic acid, 10.0 g (1 molar equivalent), was added to the resulting white suspension and the mixture was warmed to room temperature and stirred for 2 hours. The reaction mixture was poured into a container containing 100 ml of methylene chloride and 23.1 g (10 molar equivalents) of tert-butylamine while maintaining the temperature between 0-10 ° C. The mixture was stirred for 30 minutes. About 100 ml of water is added and the biphasic mixture is filtered through a Celite pad. The organic phase is separated and reduced to about half its volume by vacuum distillation. Return the solution to its original volume with acetone. Repeat this concentration / replenishment procedure twice more. The resulting acetone solution (about 300 ml) is heated to about 50 ° C and treated with about 100 ml of water to precipitate the product. The suspension was cooled and the product, 3-bromo-N (1,1-dimethylethyl) -androsta-3,5-diene-17/3-carboxamide, was isolated by filtration and dried. Yield 89%, m.p. 181-183 ° C.

(ii) 17/3-( [(1, l,dimetiletil)amino]karbonil]androsta-3,5-dien-3-karboksilna kislina(ii) 17 / 3- ([(1,1, dimethylethyl) amino] carbonyl] androsta-3,5-diene-3-carboxylic acid

Raztopino 10,0 g (1 molarni ekvivalent) 3-bromo-N-(l,l-dimetiletil)-androsta-3,5dien-17/3-karboksamida v 250 ml suhega THF segrejemo na 30 °C pod atmosfero dušika. Raztopino obdelamo z 29 ml 2,0 M etilmagnezijevega klorida (2,5 molamima ekvivalentoma) v THF, in dopustimo, da temperatura naraste na okoli 40-50°C. Po mešanju 20 minut, reakcijo ohladimo na 0-5°C in obdelamo z 82,5 ml 1,2 M sekbutillitijem v cikloheksanu (2,5 molamima ekvivalentoma). Po mešanju 5 minut, presežni suhi ogljikov dioksid vpihavamo skozi raztopino. Naplinjevanje nadaljujemo, medtem ko dopustimo, da se raztopina segreje na sobno temperaturo. Nastalo suspenzijo nato speremo s 100 ml 3,3 M vodno klorovodikovo kislino in vodno fazo odstranimo. Organosko fazo speremo dvakrat z okoli 150 ml vode. Okoli 85 ml vode dodamo organski fazi, in organsko fazo nato odstranimo z destilacijo pod znižanim tlakom. Nastalo vodno suspenzijo produkta ektrahiramo v 100 ml metil etil ketona. Vodno fazo ločimo in organsko fazo speremo s 100 ml vode. Organsko fazo obdelamo z 0,6 g razbarvalnega oglja in filtriramo skozi Celite. Uparitvi filtrata sledi trituracija v etil acetatu, da dobimo 6,4 g 17/3-[[(l,l-dimetiletil)amino]karbonil]androsta-3,5-dien-3-karboksilne kisline. Dobitek 63 %, tal. 248-249°C.A solution of 10.0 g (1 molar equivalent) of 3-bromo-N- (1,1-dimethylethyl) -androst-3,5diene-17/3-carboxamide in 250 ml of dry THF was heated to 30 ° C under a nitrogen atmosphere. The solution was treated with 29 ml of 2.0 M ethyl magnesium chloride (2.5 molar equivalents) in THF and allowed to rise to about 40-50 ° C. After stirring for 20 minutes, the reaction was cooled to 0-5 ° C and treated with 82.5 ml of 1.2 M secbutyllithium in cyclohexane (2.5 mole equivalents). After stirring for 5 minutes, excess dry carbon dioxide is bubbled through the solution. Continue pouring while allowing the solution to warm to room temperature. The resulting suspension was then washed with 100 ml of 3.3 M aqueous hydrochloric acid and the aqueous phase was removed. The organic phase is washed twice with about 150 ml of water. About 85 ml of water was added to the organic phase, and the organic phase was then removed by distillation under reduced pressure. The resulting aqueous suspension of the product was extracted into 100 ml of methyl ethyl ketone. The aqueous phase was separated and the organic phase was washed with 100 ml of water. The organic phase is treated with 0.6 g of decolourising charcoal and filtered through Celite. Evaporation of the filtrate was followed by trituration in ethyl acetate to give 6.4 g of 17/3 - [[(1,1-dimethylethyl) amino] carbonyl] androsta-3,5-diene-3-carboxylic acid. Yield 63%, m.p. 248-249 ° C.

Primer 2Example 2

3-Bromo-N-(l.l-dimetiletil)-androsta-3,5-dien-17/3-karboksamid3-Bromo-N- (1,1-dimethylethyl) -androsta-3,5-diene-17/3-carboxamide

Raztopino 10 ml metilen klorida, ki vsebuje 5 mg p-kinona, in 0,328 g (1,8 molarnega ekvivalenta) dimetilformamida ohladimo na 0°C in obdelamo z 0.85 g (1,6 molarnega ekvivalenta) oksalil bromida. Reakcijski zmesi dovolimo, da de segreje na sobno temperaturo in mešamo 30 minut. Raztopino ohladimo na okoli 5°C in beli suspenziji dodamo 0,95 g (1 molarni ekvivalent) 3-bromo-androsta-3,5-dien-17/3-karboksilne kisline v 20 ml metilen klorida. Ratopini dovolimo, da segreje na sobno temperaturo in mešamo 1,5 ure. Reakcijsko zmes prelijemo z 2,2 ml (8,4 molarnimi ekvivalenti) t-butilamina in mešamo 5 minut. Zmes zlijemo v 100 ml etil acetata in organsko fazo speremo s 50 ml 10 %-nega vodnega natrijevega hidroksida. Vodno fazo ločimo in ekstrahiramo s 50 ml etil acetata. Združene organske faze posušimo preko magnezijevega sulfata in filtriramo. Filtrat koncentriramo pod vakuumom, da dobimo surov trden produkt, ki ga trituriramo s 24 ml 50/50 t-butilmetil etra/heksana. Trden produkt izoliramo s filtracijo in posušimo pod vakuumom, da dobimo 0,5 gramaA solution of 10 ml of methylene chloride containing 5 mg of p-quinone and 0.328 g (1.8 molar equivalent) of dimethylformamide were cooled to 0 ° C and treated with 0.85 g (1.6 molar equivalent) of oxalyl bromide. The reaction mixture was allowed to warm to room temperature and stirred for 30 minutes. The solution was cooled to about 5 ° C and 0.95 g (1 molar equivalent) of 3-bromo-androst-3,5-diene-17/3-carboxylic acid in 20 ml of methylene chloride was added to the white suspension. Allow the ratopa to warm to room temperature and stir for 1.5 hours. Pour the reaction mixture with 2.2 ml (8.4 molar equivalents) of t-butylamine and stir for 5 minutes. The mixture was poured into 100 ml of ethyl acetate and the organic phase was washed with 50 ml of 10% aqueous sodium hydroxide. The aqueous phase was separated and extracted with 50 ml of ethyl acetate. The combined organic phases were dried over magnesium sulfate and filtered. The filtrate was concentrated in vacuo to give a crude solid, which was triturated with 24 ml of 50/50 t-butylmethyl ether / hexane. The solid was isolated by filtration and dried under vacuum to give 0.5 gram

3-bromo-N-(l,l-dimetiletil)-androsta-3,5-dien-17/3-karboksamida. Filtrat koncentriramo in trituriramo kot zgoraj, da dobimo nadaljnih 0,25 g produkta. Celokupni dobitek produkta je 69 %, tal. 181-183°C.3-bromo-N- (1,1-dimethylethyl) -androsta-3,5-diene-17/3-carboxamide. The filtrate was concentrated and triturated as above to give a further 0.25 g of product. The overall product yield is 69%, m.p. 181-183 ° C.

Primer 3Example 3

3-Bromoholesta-3,5-dien3-Bromocholesta-3,5-diene

Raztopino 10 ml metilen klorida, ki vsebuje 0,24 ml (1,2 molarnega ekvivalenta) dimetilformamida, ohladimo na 0°C in obdelamo z 0,62 g (1,1 molarnega ekvivalenta) oksalil bromida. Nastalo belo suspenzijo mešamo pri -5°C 45 minut in beli suspenziji dodamo 1,0 g (1 molarni ekvivalen) (+)-4-holesten-3-ona v 6 ml metilen klorida. Raztopino pustimo, da se segreje na sobno temperaturo in mešamo 30 minut. Reakcijsko zmes zlijemo v zmes 100 ml etil acetata in 40 ml vode. Organsko fazo ločimo in ekstrahiramo s 50 ml etil acetata. Združene organske faze speremo z 10 ml slanice, posušimo preko magnezijevega sulfata in filtriramo. Filtrat koncentriramo pod vakuumom, da dobimo surovi trdni produkt, ki ga prečistimo s silika gelno kromatografijo, ob uporabi heksana, da dobimo 1,1 g 3-bromoholesta-3,5diena. Dobitek 93 %. Vzorec prekristaliziramo iz metanola-dietil etra, ki ima tališče pri 64-67°C.A solution of 10 ml of methylene chloride containing 0.24 ml (1.2 molar equivalent) of dimethylformamide was cooled to 0 ° C and treated with 0.62 g (1.1 molar equivalent) of oxalyl bromide. The resulting white suspension was stirred at -5 ° C for 45 minutes and 1.0 g (1 molar equivalent) of (+) - 4-cholesten-3-one in 6 ml of methylene chloride was added to the white suspension. Allow the solution to warm to room temperature and stir for 30 minutes. The reaction mixture was poured into a mixture of 100 ml of ethyl acetate and 40 ml of water. The organic phase was separated and extracted with 50 ml of ethyl acetate. The combined organic phases were washed with 10 ml of brine, dried over magnesium sulfate and filtered. The filtrate was concentrated in vacuo to give a crude solid which was purified by silica gel chromatography using hexane to give 1.1 g of 3-bromocholesterol-3,5diene. Yield 93%. The sample was recrystallized from methanol-diethyl ether having a melting point at 64-67 ° C.

Primer 4Example 4

3-Bromo-N-(l,l-dimetiletil)-androsta-3,5-dien-17/3-karboksamid3-Bromo-N- (1,1-dimethylethyl) -androsta-3,5-diene-17/3-carboxamide

Bučko pod atmosfero dušika napolnimo z dimetilformamidom 0,6 g (2,6 molarnima ekvivalentoma) v metilen kloridu (20 ml). Raztopino ohladimo na 0-5°C in obdelamo z oksalil bromidom 1,71 g (2,5 molarnima ekvivalentoma), medtem ko vzdržujemo temperaturo med 0-10°C. Nastane bela oborina. Androst-4-en-3-on-17/3-karboksilno kislino, 1 g (1 molarni ekvivalent), dodamo nastali beli suspenziji in zmes segrejemo na blizu sobne temperature in mešamo 30 minut. Reakcijo obdelamo s tercbutilaminom, 2,2 ml (8 molarnimi ekvivalenti), v metilen kloridu (2 ml), medtem ko vzdržujemo temperaturo med 0-10°C. Reakcijo mešamo 10 minut, nato zlijemo v zmes etil acetata (150 ml) in 10 %-nega natrijevega hidroksida (50 ml). Organsko fazo ločimo, speremo s slanico, posušimo preko magnezijevega sulfata in koncentriramo, da dobimo trden produkt. Trden produkt triruriramo v raztopini t-butil metil etra (4 ml)/heksanov (4 ml), izoliramo s filtracijo in posušimo, da dobimoFill the flask under a nitrogen atmosphere with dimethylformamide 0.6 g (2.6 molar equivalents) in methylene chloride (20 ml). The solution was cooled to 0-5 ° C and treated with oxalyl bromide 1.71 g (2.5 molar equivalents) while maintaining the temperature between 0-10 ° C. A white precipitate forms. Androst-4-en-3-one-17/3-carboxylic acid, 1 g (1 molar equivalent) was added to the resulting white suspension and the mixture was warmed to near room temperature and stirred for 30 minutes. The reaction was treated with tert-butylamine, 2.2 ml (8 molar equivalents), in methylene chloride (2 ml), while maintaining the temperature between 0-10 ° C. The reaction was stirred for 10 minutes, then poured into a mixture of ethyl acetate (150 ml) and 10% sodium hydroxide (50 ml). The organic phase was separated, washed with brine, dried over magnesium sulfate and concentrated to give a solid product. The solid was triturated in a solution of t-butyl methyl ether (4 ml) / hexanes (4 ml), isolated by filtration and dried to give

3-Bromo-N-(l,l-dimetiletil)-androsta-3,5-dien-17j3-karboksamid. Dobitek je 58 %. Tal. 177-179°C.3-Bromo-N- (1,1-dimethylethyl) -androsta-3,5-diene-17 H -carboxamide. The yield is 58%. Tal. 177-179 ° C.

Claims (24)

Patentni zahtevkiPatent claims 1. Postopek za pripravo spojine s formulo (I)A process for the preparation of a compound of formula (I) OOh G v kateri:G in which: je R1 NR3R4, kjer R3 in R4 vsakega neodisno izberemo izmed vodika, alkila, C3g5 cikloalkila, fenila; ali R3 in R4 skupaj z dušikom, na katerega sta vezana, predstavljata 5-6 členski nasičen obroč, ki vsebuje do en drug heteroatom, izbran izmed kisika in dušika; in je R2 kislina ali ester;R 1 is NR 3 R 4 , wherein R 3 and R 4 are each independently selected from hydrogen, alkyl, C 3-5 cycloalkyl, phenyl; or R 3 and R 4 together with the nitrogen to which they are attached represent a 5-6 membered saturated ring containing up to one heteroatom selected from oxygen and nitrogen; and R 2 is an acid or ester; ali njene farmacevtsko sprejemljive soli, hidrata ali solvata, označen s tem, daor a pharmaceutically acceptable salt, hydrate or solvate thereof, characterized in that a) presnovimo, pri znižani temperaturi, spojino s formulo (II)a) at reduced temperature, the compound of formula (II) is reacted O (II) v prisotnosti halogen-Vilsmeierjevega reagenta in topila, nato prekinemo reakcijo s prebitnim H-R1, kjer je R1, kot je definirano prej, da dobimo spojino s formulo (III) v kateri je halogen brom ali jod; in je R1, kot je definirano zgoraj, inO (II) in the presence of a halogen-Vilsmeier reagent and solvent, is then terminated by reaction with excess HR 1 , wherein R 1 is as previously defined to give a compound of formula (III) wherein halogen is bromine or iodine; and R 1 is as defined above and b) naknadno, v primernem topilu in pri znižani temperaturi, dodamo alikillitijev reagent, ki mu sledi pripajalni reagent, da dobimo spojino s formulo (I), da kadar je R3 in/ali R4 H, podvržemo spojino s formulo (III) bazičnemu mediju, primernemu za selektivno deprotoniranje amida, predno dodamo alikillitijev reagent in nato v danem primeru pripravimo farmacevtsko sprejemljivo sol, hidrat ali solvat.b) subsequently, in a suitable solvent and at reduced temperature, an allycyl lithium reagent, followed by a coupling reagent, is added to give the compound of formula (I) to subject the compound of formula (III) when R 3 and / or R 4 H. to a basic medium suitable for the selective deprotonation of the amide, prior to the addition of an allycyl lithium reagent and then optionally preparing a pharmaceutically acceptable salt, hydrate or solvate. 2. Postopek po zahtevku 1, označen s tem, da halogen-Vilsmeierjev reagent pripravimo s presnovitvijo, prednostno pri znižanih temperaturah, kloridnega vira, kot je oksalil klorid ali tionil klorid, z disubstituiranim formamidnim reagentom, kot je dialkil substituirani formamidni reagent, prednostno dimetil formamid, v primernem topilu, prednostno metilen kloridu, da dobimo kloroVilsmeierjev reagent, pri čemer omenjeni kloro-Vilsmeirejev reagent prenovimo, prednostno pri znižanih temperaturah, z bromidnim virom ali jodidnim virom, prednostno s plinskim bromovodikom.Process according to claim 1, characterized in that the halogen-Wilsmeier reagent is prepared by metabolizing, preferably at reduced temperatures, a chloride source such as oxalyl chloride or thionyl chloride with a disubstituted formamide reagent such as dialkyl substituted formamide reagent, preferably dimethyl formamide, in a suitable solvent, preferably methylene chloride, to give the chloroVilsmeier reagent, said chloro-Wilsmeire reagent being reacted, preferably at reduced temperatures, with a bromide source or an iodide source, preferably with a gas bromide hydrogen gas. 3. Postopek po zahtevku 2, označen s tem, da je halogen-Vilsmeierjev reagent bromo-Vilsmeierjev reagent.Process according to claim 2, characterized in that the halogen-Vilsmeier reagent is a bromo-Vilsmeier reagent. 4. Postopek po zahtevku 2, označen s tem, da je halogen-Vilsmeierjev reagent jodo-Vilsmeierjev reagent.Process according to claim 2, characterized in that the halogen-Vilsmeier reagent is an iodo-Vilsmeier reagent. 5. Postopek po zahtevku 3, označen s tem, da je bromo-Vilsmeierjev reagent (bromometilen) dimetil amonijev bromid.Process according to claim 3, characterized in that the bromo-Wilsmeier reagent is (bromomethylene) dimethyl ammonium bromide. 6. Postopek po zahtevku 2, označen s tem, da je R2:A process according to claim 2, characterized in that R 2 is : -SO3H, -P(O)(OH)2, -PH(O)(OH) ali -(CH^COOH.-SO 3 H, -P (O) (OH) 2 , -PH (O) (OH) or - (CH 2 COOH. 7. Postopek po zahtevku 2, označen s tem, da je R2 -COOH.The process of claim 2, wherein R 2 is -COOH. 8. Postopek po zahtevku 2, označen s tem, da bazo, ki jo uporabimo za pripravo bazičnega medija, izberemo iz skupine, ki se sestoji predvsem iz: hidridov, alkil litija, gringnardovih reagentov in kovinskih alkoksidov.Process according to claim 2, characterized in that the base used for the preparation of the basic medium is selected from the group consisting mainly of: hydrides, alkyl lithium, gringnard reagents and metal alkoxides. 9. Postopek po zahtevku 8, označen s tem, da je baza etilmagnezijev bromid ali etilmagnezijev klorid.A process according to claim 8, characterized in that the base is ethylmagnesium bromide or ethylmagnesium chloride. 10. Postopek po zahtevku 9, označen s tem, da je baza etilmagnezijev klorid.A process according to claim 9, characterized in that the base is ethylmagnesium chloride. 11. Postopek po zahtevku 2, označen s tem, daje alkillitijev reagent sek-butillitij.11. The process of claim 2, wherein the alkyllithium reagent is sec-butyllithium. 12. Postopek po zahtevku 2, označen s tem, da je R1 -N(H)C(CH3)3.A process according to claim 2, wherein R 1 is -N (H) C (CH 3 ) 3 . 13. Postopek po zahtevku 2, označen s tem, da pripravimo spojinoProcess according to claim 2, characterized in that a compound is prepared OOh II ali njeno farmacevtsko sprejemljivo sol, hidrat ali solvat.II or a pharmaceutically acceptable salt, hydrate or solvate thereof. 14. Postopek za pripravo steroidnega karboksamidnega substituenta, označen s tem, da halogeniramo ustrezno karboksilno kislino s halogen-Vilsmeierjevim reagentom, nakar reakcijo prekinemo s prebitnim H-R1, kjer je R1 NR3R4, kjer R3 in R4 vsakega neodvisno izberemo izmed vodika, g alkila, C3^ cikloalkila, fenila; ali R3 in R4 skupaj z dušikom, na katerega sta vezana, predstavljata 5-6 členski nasičen obroč, ki vključuje do en drug heteroatom, izbran izmed kisika in dušika.14. A process for the preparation of a steroid carboxamide substituent, characterized in that the corresponding carboxylic acid is halogenated with a halogen-Vilsmeier reagent and then terminated with excess HR 1 , wherein R 1 is NR 3 R 4 , wherein R 3 and R 4 are each independently selected from hydrogen, g alkyl, C 3 ^ cycloalkyl, phenyl; or R 3 and R 4 together with the nitrogen to which they are attached represent a 5-6 membered saturated ring which includes up to one heteroatom selected from oxygen and nitrogen. 15. Postopek po zahtevku 14, označen s tem, da halogen-Vilsmeierjev reagent pripravimo s presnovitvijo, prednostno pri znižanih temperaturah, kloridnega vira, kot je oksalil klorid ali tionil klorid, s disubstituiranim formamidnim reagentom, kot je dialkil substituirani formamidni reagent, pprednostno dimetilformamid, v primernem topilu, prednostno metilen kloridu, da dobimo kloroVilsmeierjev reagent, pri čemer omenjeni kloro-Vilsemierjev reagent presnovimo in situ, prednostno pri znižanih temperaturah, z bromidnim virom ali jodidnim virom, prednostno s plinskim bromovodikom.Process according to claim 14, characterized in that the halogen-Wilsmeier reagent is prepared by metabolizing, preferably at reduced temperatures, a chloride source such as oxalyl chloride or thionyl chloride with a disubstituted formamide reagent, such as dialkyl substituted formamide reagent, preferably dimethylformyl , in a suitable solvent, preferably methylene chloride, to give the chloroVilsmeier reagent, said chloro-Wilsemier reagent being reacted in situ, preferably at reduced temperatures, with a bromide source or an iodide source, preferably with a gas bromine hydrogen gas. 16. Postopek po zahtevku 15, označen s tem, da je halogen brom.A process according to claim 15, characterized in that it is halogen bromine. 17. Postopek po zahtevku 16, označen s tem, da bromo-Vilsmeierjev reagent pripravimo in uporabimo in situ.Process according to claim 16, characterized in that the bromo-Wilsmeier reagent is prepared and used in situ. 18. Postopek po zahtevku 17, označen s tem, da je bromo-Vilsmeierjev reagent (bromometilen) dimetil amonijev bromid.18. The process according to claim 17, wherein the bromo-Wilsmeier reagent is (bromomethylene) dimethyl ammonium bromide. 19. Postopek za pripravo steroidnih halo-l,3-dienov, označen s tem, da halogeniramo odgovarjajoči α,/3-nenasičeni keton s halogen-Vilsmeierjevim reagentom.19. A process for the preparation of steroidal halo-1,3-dienes, characterized in that the corresponding α, / 3-unsaturated ketone is halogenated with a halogen-Vilsmeier reagent. 20. Postopek po zahtevku 19, označen s tem, da halogen-Vilsmeierjev reagent pripravimo s presnovitvijo, prednostno pri znižanih temperaturah, kloridnega vira, kot je oksalil klorid ali tionil klorid, z disubstituiranim formamidnim reagentom, kot je dialkil substituirani formamidni reagent, prednostno dimetilformamid, v primernem topilu, prednostno metilen kloridu, da dobimo kloroVilsmeierjev reagent, pri čemer omenjeni kloro-Vilsmeierjev reagent presnovimo in situ, prednostno pri znižanih temperaturah, z bromidnim virom ali jodidnim virom, prednostno plinskim bromovodikom.Process according to claim 19, characterized in that the halogen-Wilsmeier reagent is prepared by metabolizing, preferably at reduced temperatures, a chloride source such as oxalyl chloride or thionyl chloride with a disubstituted formamide reagent such as dialkyl substituted formamide reagent, preferably dimethylformamide , in a suitable solvent, preferably methylene chloride, to obtain the chloroVilsmeier reagent, said chloro-Wilsmeier reagent being reacted in situ, preferably at reduced temperatures, with a bromide source or an iodide source, preferably a gas bromine hydrogen gas. 21. Postopek po zahtevku 20, označen s tem, da je pripravljena spojina steroidni bromo-l,3-dien.21. The method of claim 20, wherein the compound is steroid bromo-1,3-diene. 22. Postopek po zahtevku 21, označen s tem, da je pripravljena spojina 3-bromo-3,5dien.The process of claim 21, wherein the compound is 3-bromo-3,5diene. 23. Postopek po zahtevku 22, označen s tem, da je halogen-Vilsmeierjev reagent (bromometilen) dimetil amonijev bromid.A process according to claim 22, characterized in that the halogen-Wilsmeier reagent is (bromomethylene) dimethyl ammonium bromide. 23. Postopek za halogenacijo mnogovrstnih funkcionalnih skupin na eni molekuli, označen s tem, da halogeniramo molekulo z mnogovrstnimi funkcionalnimi skupinami s halogen-Vilsmeierjevim reagentom.23. A process for halogenating multiple functional groups on a single molecule, characterized in that the molecule is halogenated with multiple functional groups with a halogen-Vilsmeier reagent. 25. Postopek po zahtevku 24, označen s tem, da halogen-Vilsmeierjev reagent pripravimo s presnovitvijo, prednostno pri znižanih temperaturah, kloridnega vira, kot je oksalil klorid ali tionil klorid, z disubstituiranim formamidnim reagentom, kot je dialkil substituirani formamidni reagent, prednostno dimetilformamid, v primernem topilu, prednostno metilen kloridu, da dobimo kloroVilsmeierjev reagent, omenjeni kloro-Vilsmeieijev reagent presnovimo in situ, prenostno pri znižanih temperaturah, z bromidnim virom ali jodidnim virom, prenostno plinskim bromovodikom.Process according to claim 24, characterized in that the halogen-Wilsmeier reagent is prepared by metabolizing, preferably at reduced temperatures, a chloride source such as oxalyl chloride or thionyl chloride with a disubstituted formamide reagent such as dialkyl substituted formamide reagent, preferably dimethylformamide , in a suitable solvent, preferably methylene chloride, to obtain the chloroVilsmeier reagent, said chloro-Vilsmeie reagent is reacted in situ, preferably at reduced temperatures, with a bromide source or an iodide source, preferably a gas bromine hydrogen chloride.
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