首页> 外国专利> DERIVATIVES OF 1'-(2-HYDROXY-3-ARYLOXYPROPYL-1-YL)-SUBSTITUTED SPIROBENZOFURAN-PIPERIDINES, SPIROBENZOFURAN-PYRROLIDINES AND SPIROCHROMEN-PIPERIDINES, METHOD FOR THEIR PREPARING, INTERMEDIATE COMPOUND AND METHOD FOR ITS PREPARING, PHARMACEUTICAL COMPOSITION, USING

DERIVATIVES OF 1'-(2-HYDROXY-3-ARYLOXYPROPYL-1-YL)-SUBSTITUTED SPIROBENZOFURAN-PIPERIDINES, SPIROBENZOFURAN-PYRROLIDINES AND SPIROCHROMEN-PIPERIDINES, METHOD FOR THEIR PREPARING, INTERMEDIATE COMPOUND AND METHOD FOR ITS PREPARING, PHARMACEUTICAL COMPOSITION, USING

机译：1'-（2-羟基-3-芳氧丙基-1-基）取代的螺[苯并呋喃-吡咯烷酮]，螺[苯并呋喃-吡咯烷酮]和螺[铬-哌啶酮]的衍生物，其制备方法，中间化合物和方法用于其制备，药物成分，使用

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FIELD: organic chemistry, medicine, pharmacy.;SUBSTANCE: invention relates to compounds of the formula (I): their using (variants) for preparing a drug used in treatment of diseases modulation of activity of chemokine receptors is useful, and to a pharmaceutical composition modulating chemokine receptors and comprising abovementioned compound. In compound of the formula (I) m = 0 or 1; R¹ means halogen atom; X, Y and Z represent independently a bond, -CH₂- or -O-, or X and Y form in common -CH=C(CH₃)- or -C(CH₃)=CH- under condition that only one radical among X, Y and Z can represents a bond, and under condition that X and Y both don't represent -O- simultaneously; n = 0, 1 or 2; R² represents halogen atom, or (C₁-C₆)-alkyl; q = 0 or 1; R³ represents -NHC(O)R¹⁰, -C(O)NR¹¹R¹² or -COOR^12a; each radical among R⁴, R⁵, R⁶, R⁷ and R⁸ represents independently hydrogen atom (H) or (C₁-C₆)-alkyl; t = 0, 1 or 2; R⁹ represents halogen atom, -OH, -COOH, (C₁-C₆)-alkoxy group, (C₁-C₆)-alkoxycarbonyl; R¹⁰ represents group (C₁-C₆)-alkyl, (C₃-C₆)-cycloalkyl, or R¹⁰ represents -NR¹⁴R¹⁵; each R¹¹ and R¹² represents independently (1) H; (2) 3-6-membered saturated cycloalkyl or phenyl or 5-membered unsaturated heterocyclyl comprising from 1 to 4 heteroatoms N wherein indicated cycloalkyl, phenyl and heterocyclyl are substituted possibly with one or two substitutes chosen from -OH, (C₁-C₆)-alkyl, (C₁-C₆)-hydroxyalkyl; (3) (C₁-C₆)-alkyl substituted possibly at least with one substitute chosen from halogen atom, -OH, -COOH, (C₁-C₆)-alkylcarbonylamino group, phenyl, 5-membered unsaturated heterocyclyl comprising oxygen atom (O), or from 1 to 2 N atoms, bicycloheptyl wherein this phenyl, heterocyclyl or bicycloheptyl is substituted possibly at least with one substitute chosen from halogen atom, -OH, =O, or (4) (C₁-C₆)-alkylsulfonyl, or R¹¹ and R¹² in common with N atoms to which they are bound form 5-membered unsaturated heterocyclyl comprising one N atom or 5-6-membered heterocyclyl comprising from 1 to 2 heteroatoms, such as S, O and N, or 5-6-membered saturated heterocyclyl, ortho-condensed with benzene ring and comprising one N atom and wherein indicated heterocyclic systems are substituted possibly with one or two substitutes chosen from halogen atom, (C₁-C₆)-alkyl, (C₁-C₆)-hyroxyalkyl, (C₁-C₆)-halogenalkyl, (C₁-C₆)-alkylamino, di-(C₁-C₆)-alkylamino group, phenyl, halogenphenyl and hydroxydiphenylmethyl; R^12a represents H or (C₁-C₆)-alkyl; each radical among R¹⁴ and R¹⁵represents independently H or (C₁-C₆)-alkylsulfonyl, or R¹⁴ and R¹⁵ in common with N atom to which they are bound form 5-membered saturated heterocyclyl comprising one N atom and substituted possibly with one -OH, or its pharmaceutically acceptable salt or solvate. Also, invention relates to a method (variants) for synthesis of compound of the formula (I) according to one of the following method: by one variant, compound of the formula (II): is subjected for interaction with compound of the formula (III): by other variant, compound of the formula (IV): is subjected for interaction with compound of the formula (V): by other variant, compound of the formula (VI): wherein R³ represents -NHC(O)R¹⁰ and L¹ represents a leaving group is subjected for interaction with L¹C(O)R¹⁰; by other variant, compound of the formula (VIII): wherein R³represents -C(O)NR¹¹R¹² and L² represents a leaving group is subjected for interaction with compound of the formula (IX) given in the invention description. Also, invention relates to an intermediate compound of the formula (IIA): (wherein R^1a is chosen from F, Cl, -CH₃ and -CF₃; s = 1 or 2; q = 0 or 1; w = 0 or 1; R^2a represents F, and when q and s = 1 and w = 0 then R^1a can't represent chlorine atom), and to a method for synthesis of compound of the formula (IIA) (wherein s = 1) and wherein compound of the formula (XX): is subjected for interaction with compound of the formula (XXII): (wherein R²⁰ represent a protective group) before formation of compound of the formula (XXIV): followed by carrying out the cyclization reaction and removing the protective group R²⁰.;EFFECT: improved methods of synthesis.;25 cl, 236 ex

机译：技术领域本发明涉及式（I）的化合物：<图像文件=“ 00000012.GIF” he =“ 36” imgContent =“ undefined” imgFormat =“ GIF” wi =“ 122″其用于制备治疗疾病的药物的用途（变体）用于调节趋化因子受体的活性，并且对调节趋化因子受体的药物组合物有用并且包含上述化合物。在式（I）的化合物中，m = 0或1; R ^{1 表示卤素原子; X，Y和Z独立代表一个键，-CH _{2 -或-O-或X和Y形式的常见-CH = C（CH _{3 ）-或-C（CH _{3 ）= CH-在X，Y和Z中仅一个基团可以表示键的条件下，并且在X和Y都不同时表示-O-的条件下; n = 0、1或2; R ^{2 代表卤素原子，或（C _{1 -C _{6 ）-烷基; q = 0或1; R ^{3 代表-NHC（O）R ^{10 ，-C（O）NR ^{11 R ^{12 或- COOR ^{12a ; R ^{4 ，R ^{5 ，R ^{6 ，R ^{7 和R ^{8 独立地表示氢原子（H）或（C _{1 -C _{6 ）-烷基; t = 0、1或2; R ^{9 代表卤素原子，-OH，-COOH，（C _{1 -C _{6 ）-烷氧基，（C _{1 -C _{6 ）-烷氧羰基; R ^{10 代表基团（C _{1 -C _{6 ）-烷基，（C _{3 -C _{6 ）-环烷基，或R ^{10 代表-NR ^{14 R ^{15 ; R ^{11 和R ^{12 分别独立地表示（1）H; （2）包含1-4个杂原子N的3-6元饱和环烷基或苯基或5元不饱和杂环基，其中所示的环烷基，苯基和杂环基可能被选自-OH的一个或两个取代基取代（C _{1 -C _{6 ）-烷基，（C _{1 -C _{6 ）-羟烷基; （3）（C _{1 -C _{6 ）-烷基，可能至少被一个选自卤素原子，-OH，-COOH的取代基取代，（C _{1 -C _{6 ）-烷基羰基氨基，苯基，包含氧原子（O）或1至2个N原子的5元不饱和杂环基，双环庚基，其中该苯基，杂环基或双环庚基为可能至少被一个选自卤素原子，-OH，= O或（4）（C _{1 -C _{6 ）-烷基磺酰基的取代基取代，或R ^{11 和R ^{12 与它们所键合的N原子共同形成包含一个N原子的5元不饱和杂环基或包含1-2个杂原子的5-6元杂环基，诸如S，O和N，或5-6元饱和杂环基，其与苯环邻位缩合并包含一个N原子，并且其中所示的杂环系统可能被选自卤素原子的一个或两个取代基取代，（C _{1 -C _{6 ）-烷基，（C _{1 -C _{6 ）-羟烷基，（C _{1 -C _{6 ）-卤代烷基，（C _{1 -C _{6 ）-烷基氨基，二-（C _{1 -C _{6 ）-烷基氨基，苯基，卤代苯基和羟基二苯基甲基; R ^{12a 代表H或（C _{1 -C _{6 ）-烷基; R ^{14 和R ^{15 中的每个基团独立地代表H或（C _{1 -C _{6 ）-烷基磺酰基，或与它们所键合的N原子共同的R ^{14 和R ^{15 形成包含一个N原子并可能被一个-OH取代的5元饱和杂环基，或其药学上可接受的盐或溶剂化物。另外，本发明涉及一种根据以下方法之一合成式（I）的化合物的方法（变体）：通过一个变体，式（II）的化合物：与式（III）的化合物发生相互作用：，由其他变体（公式（IV）的化合物）组成：<图像文件=“ 00000015.GIF” he =“ 36” imgContent =“ undefined” imgFormat =“ GIF “ wi =“ 102” />与式（V）的化合物发生相互作用：通过其他变式，由式（VI）的化合物组成：其中R ^{3 代表-NHC（O）R ^{10 ，L ^{1 代表离去基团与L ^{1 C相互作用（ O）R ^{10 ;另一变体，是式（VIII）的化合物：其中R ^{3 < / Sup>表示-C（O）NR ^{11 R ^{12 ，L ^{2 表示离去基团与下式的化合物相互作用（IX）在发明说明书中给出。也，本发明涉及式（IIA）的中间体化合物：<图像文件=“ 00000019.GIF” he =“ 32” imgContent =“ undefined” imgFormat =“ GIF” wi =“ 63” />（其中R ^{1a 选自F，Cl，-CH _{3 和-CF _{3 ; s = 1或2; q = 0或1; w = 0或1; R ^{2a 代表F，当q和s = 1且w = 0时，R ^{1a 不能代表氯原子），并合成式（IIA）的化合物（其中s = 1），其中式（XX）的化合物：与式（XXII）的化合物相互作用：（其中R ^{20 代表保护基）在形成式（XXIV）的化合物之前：，然后进行环化反应并除去脯氨酸保护组R ^{20 。;效果：改进的合成方法。; 25 cl，236 ex}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}}

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公开/公告号RU2320664C2

专利类型
公开/公告日2008-03-27

原文格式PDF
申请/专利权人 ASTRAZENEKA AB;
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申请/专利号RU20040137278
发明设计人 KHOSSAIN NAFIZAL (SE);IVANOVA SVETLANA (SE);MONSONIDES-KHARSEMA MARGERITE (SE);
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申请日2003-07-07
分类号C07D491/10;C07D471/10;C07D221/20;C07D209/54;
国家 RU
入库时间 2022-08-21 19:50:44

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