会员体验
专利管家(专利管理)
工作空间(专利管理)
风险监控(情报监控)
数据分析(专利分析)
侵权分析(诉讼无效)
联系我们
交流群
官方交流:
QQ群: 891211   
微信请扫码    >>>
现在联系顾问~
热词
    • 2. 发明授权
    • 20-alkyl-7-oxoprostacyclin derivatives useful as pharmaceuticals
    • 可用作药物的20-烷基-7-氧代前列环素衍生物
    • US5190973A
    • 1993-03-02
    • US599916
    • 1990-10-19
    • Robert NickolsonHelmut VorbrueggenClaus S. StuerzebecherMartin Haberey
    • Robert NickolsonHelmut VorbrueggenClaus S. StuerzebecherMartin Haberey
    • C07C405/00C07D307/935C07D307/937
    • C07D307/935C07C405/00C07D307/937
    • The invention concerns 20-alkyl-7-oxoprostacyclin derivatives of general Formula I ##STR1## wherein R.sub.1 is the residue OR.sub.3 where R.sub.3 means hydrogen or alkyl of 1-10 carbon atoms optionally substituted by halogen, phenyl, C.sub.1 -C.sub.4 -alkoxy or C.sub.1 -C.sub.4 -dialkylamino; cycloalkyl, aryl or a heterocyclic residue, or the residue NHR.sub.4 where R.sub.4 means hydrogen or an alkanoyl or alkanesulfonyl residue of respectively 1-10 carbon atoms,n is 1 or 2,A is a CH.sub.2 --CH.sub.2 --, cis--CH.dbd.CH-- or trans--CH.dbd.CH--group,W is a ##STR2## or a ##STR3## wherein the OH-group can respectively be esterified with a benzoyl or alkanoic acid residue of 1-4 carbon atoms, or etherified with a tetrahydropyranol, tetrahydrofuranyl, alkoxyalkyl or trialkylsilyl residue, wherein the free or esterified OH-group can be in the .alpha.- or .beta.-position,R.sub.2 is a straight-chain or branched-chain alkyl group of 1-6 carbon atoms,R.sub.5 is a hydroxy group which can be esterified with an alkanoic acid residue of 1-4 carbon atoms or etherified with a tetrahydropyranyl, tetrahydrofuranyl, alkoxyalkyl or trialkylsilyl residue,R.sub.6 and R.sub.7 are hydrogen or a straight-chain or branched-chain alkyl group of 1-4 carbon atoms, or R.sub.6 and R.sub.7 jointly represent a trimethylene group,R.sub.8 and R.sub.9 jointly represent a linkage or hydrogen or a straight-chain or branched-chain alkyl group of 1-4 carbon atoms,and, if R.sub.3 is hydrogen, the salts thereof with physiologically compatible bases; their production; and their use as medicinal agents.
    • 本发明涉及通式I(I)的20-烷基-7-氧代前列环素衍生物,其中R 1是残基OR 3,其中R 3表示氢或1-10个碳原子的任选被卤素,苯基,C 1 -C 4 - 烷氧基或C 1 -C 4 - 二烷基氨基; 环烷基,芳基或杂环残基,或残基NHR4,其中R4表示氢或分别为1-10个碳原子的烷酰基或烷磺酰基,n为1或2,A为CH2-CH2-,顺式-CH = CH- 或反式-CH = CH-基团,W为“IMAGE”或“IMAGE”,其中OH基团可分别用1-4个碳原子的苯甲酰基或链烷酸残基酯化,或用四氢吡喃醇醚化,四氢呋喃基 ,烷氧基烷基或三烷基甲硅烷基残基,其中游离或酯化的OH基可以是α或β-位,R2是1-6个碳原子的直链或支链烷基,R5是羟基, 可以用1-4个碳原子的链烷酸残基酯化,或与四氢吡喃基,四氢呋喃基,烷氧基烷基或三烷基甲硅烷基残基醚化,R6和R7是氢或1-4个碳原子的直链或支链烷基, 或R6和R7共同表示三亚甲基,R8和R9共同表示键或 氢或1-4个碳原子的直链或支链烷基,如果R 3是氢,则其与生理上相容的碱的盐; 他们的生产; 并将其用作药剂。
    • 4. 发明授权
    • 5.beta.-Hydroxy-.DELTA..sup.6 -steroids and process for the preparation
thereof
    • 5β-羟基-DTATA 6-类固醇及其制备方法
    • US4472310A
    • 1984-09-18
    • US359713
    • 1982-03-11
    • Dieter BittlerHenry LaurentKlaus NickischRobert NickolsonRudolf Wiechert
    • Dieter BittlerHenry LaurentKlaus NickischRobert NickolsonRudolf Wiechert
    • C07J1/00C07J21/00C07J53/00C07J71/00
    • C07J21/003C07J1/0025C07J53/008C07J71/001
    • The disclosure concerns 5.beta.-hydroxy-.DELTA..sup.6 -steroids of the general formula ##STR1## wherein R.sup.1 is hydrogen, acyl, lower alkyl, or the tetrahydropyranyl residue andR.sup.2, R.sup.3 individually are respectively hydrogen or jointly are methylene andX stands for oxygen, the groupings ##STR2## (wherein R.sup.4 means hydrogen or acyl) and ##STR3## (wherein R.sup.5 means hydrogen or lower alkyl) and a process for the preparation thereof by reacting corresponding 7.alpha.-chloro-5.beta.,6.beta.-epoxy steroids in an inert solvent with metallic zinc in a lower aliphatic carboxylic acid or dilute mineral acid at temperatures of between room temperature and 100.degree. C., preferably at 40.degree.-70.degree. C.The compounds producible by this method are intermediates for the preparation of 3-keto-.DELTA..sup.4 -6.beta.,7.beta.-methylene steroids constituting pharmacologically valuable compounds, for example aldosterone antagonists.
    • PCT No.PCT / DE81 / 00111 Sec。 371日期1982年3月11日 102(e)1982年3月11日PCT PCT。 公开号WO82 / 00294 日本1982年2月4日。该公开内容涉及通式为“IMAGE”的5ββ-羟基-DTATA-类固醇,其中R 1为氢,酰基,低级烷基或四氢吡喃基,R2,R3分别为氢或共同 (其中R 4表示氢或酰基)和(其中R 5表示氢或低级烷基)及其制备方法,通过使相应的7α- 氯代-5β,6β-环氧类固醇在惰性溶剂中与金​​属锌在低级脂族羧酸或稀无机酸中在室温至100℃之间,优选40℃-70℃的温度下进行。化合物 通过该方法可生产的是制备构成药理学上有价值的化合物的3-酮-TATA4-6β,7β-亚甲基甾族化合物的中间体,例如醛固酮拮抗剂。
    • 7. 发明授权
    • Process for the preparation of 21-hydroxy-16-pregnen-20-one derivatives
    • 制备21-羟基-16-孕烯-20-酮衍生物的方法
    • US4089852A
    • 1978-05-16
    • US682967
    • 1976-05-04
    • Robert Nickolson
    • Robert Nickolson
    • C07J1/00C07J13/00C07J17/00
    • C07J13/005C07J1/0033C07J17/00
    • .DELTA..sup.16 -21-HYDROXY-20-KETO STEROIDS OF THE PREGNANE SERIES HAVING AN OTHERWISE UNSUBSTITUTED D-ring and a 13-methyl or -ethyl group, and 21-ethers and -esters thereof, are produced by reaction of a corresponding D-ring saturated 17-keto steroid with a lithium compound of the formula ##STR1## thereby converting the 17-keto group to a 17.beta.-hydroxy-20.alpha.-enol ether in which the 17.alpha.-side chain has the formula ##STR2## wherein R.sub.3 and R.sub.4 have the values given above, and, in any desired sequence, splitting off R.sub.3 and/or R.sub.4 enol ether by hydrolysis; eliminating 17.beta.-hydroxy group, preferably after acylation, with formation of a .DELTA..sup.16 -double bond; and, if desired, splitting off any blocking group.
    • 具有其他不分离的D-环和13-甲基或乙基的PREGNANE系列的DELTA 16-21-羟基-20-酮酸类固醇及其21-醚和 - 酯通过相应的D- 环状饱和的17-酮类固醇与式“IMAGE”的锂化合物反应,从而将17-酮基转化为17β-羟基-20α-烯醇醚,其中17α-侧链具有式,其中 R3和R4具有上述给出的值,并且以任何所需的顺序通过水解分离R3和/或R4烯醇醚; 消除17个β-羟基,优选在酰化后,形成DELTA16-双键; 并且如果需要,分解任何封闭基团。