公开(公告)号：WO2004032967A8

公开(公告)日：2005-05-06

申请号：PCT/FR0302986

申请日：2003-10-10

Applicant: SERVIER LAB ,  CENTRE NAT RECH SCIENT ,  CASTEILLA LOUIS ,  PENICAUD LUC ,  DACQUET CATHERINE ,  RENARD PIERRE

Inventor： CASTEILLA LOUIS ,  PENICAUD LUC ,  DACQUET CATHERINE ,  RENARD PIERRE

IPC: A61K45/06 ,  A61P3/04 ,  A61P3/10 ,  A61K31/122 ,  A61K31/4439

CPC classification number: A61K31/122 ,  A61K31/4439 ,  A61K45/06 ,  A61K2300/00

Abstract: The invention concerns an association containing one or more ligands of the peroxisome proliferator activated receptors and an antioxidant agent. The invention is applicable to medicines.

Abstract translation: 本发明涉及含有一种或多种过氧化物酶体增殖物激活受体配体和抗氧化剂的结合物。 本发明适用于药物。

公开(公告)号：WO2004048340A8

公开(公告)日：2005-07-07

申请号：PCT/EP0314841

申请日：2003-11-26

Applicant: SHANGHAI INST MATERIA MEDICA ,  SERVIER LAB ,  QIN GUO-WEI ,  TANG XI-CAN ,  WANG RUI ,  ZHOU TIAN-XI ,  LESTAGE PIERRE ,  CAIGNARD DANIEL-HENRI ,  RENARD PIERRE

Inventor： QIN GUO-WEI ,  TANG XI-CAN ,  WANG RUI ,  ZHOU TIAN-XI ,  LESTAGE PIERRE ,  CAIGNARD DANIEL-HENRI ,  RENARD PIERRE

IPC: C07D221/28 ,  A61K31/485 ,  C07D489/00

CPC classification number: C07D221/28

Abstract: The invention relates to sinomenine and compounds thereof and also to compounds of formula (I), wherein R1 represents an alkyl group; R2 represents a hydrogen atom or an alkylcarbonyl group, an haloalkylcarbonyl group or an arylcarbonyl; Y represents a group (II), (III) or (IV); R3 ,R4, R'4, R5, R'5 and R6 are as defined in the description; and X represents a halogen atom. Medicaments.

Abstract translation: 本发明涉及青藤碱及其化合物，还涉及式（I）化合物，其中R 1表示烷基; R2表示氢原子或烷基羰基，卤代烷基羰基或芳基羰基; Y代表（II），（III）或（IV）; R3，R4，R'4，R5，R'5和R6如说明书中所定义; X表示卤素原子。 药物。

公开(公告)号：JP2003089639A

公开(公告)日：2003-03-28

申请号：JP2002196850

申请日：2002-07-05

Applicant: SERVIER LAB

Inventor： LANGLOIS MICHEL ,  MATHE-ALLAINMAT MONIQUE ,  LEFAS-LE GALL MARIE ,  BENNEJEAN CAROLINE ,  RENARD PIERRE ,  DELAGRANGE PHILIPPE

IPC: C07D339/00 ,  A61K31/16 ,  A61K31/165 ,  A61K31/17 ,  A61K31/335 ,  A61K31/343 ,  A61K31/352 ,  A61K31/353 ,  A61K31/38 ,  A61K31/381 ,  A61K31/395 ,  A61K31/4355 ,  A61K31/437 ,  A61P1/00 ,  A61P3/04 ,  A61P3/10 ,  A61P9/00 ,  A61P15/00 ,  A61P25/00 ,  A61P25/04 ,  A61P25/06 ,  A61P25/08 ,  A61P25/16 ,  A61P25/18 ,  A61P25/20 ,  A61P25/22 ,  A61P25/24 ,  A61P25/28 ,  A61P35/00 ,  A61P43/00 ,  C07C233/18 ,  C07C233/23 ,  C07C233/74 ,  C07C235/34 ,  C07C235/40 ,  C07C275/26 ,  C07D307/79 ,  C07D307/80 ,  C07D307/81 ,  C07D311/92 ,  C07D333/58 ,  C07D333/60 ,  C07D471/04 ,  C07D491/04 ,  C07D491/048 ,  C07D493/04

Abstract: PROBLEM TO BE SOLVED: To obtain a new cyclic compound having pharmacological action on the receptor for a compound having melatonin-like activity. SOLUTION: This new cyclic compound is expressed by formula (I) [R is ORa , SRa , Ra or a cyclic group; A is a cyclic structure group; G1 and G2 are each an alkylene chain or a single bond; B is NR a C(Q)R a , NR a C(Q)NR a R a or C(Q)NR a R a ; and (p) and (q) are numbers satisfying the formula 1

公开(公告)号：JP2002179652A

公开(公告)日：2002-06-26

申请号：JP2001319183

申请日：2001-10-17

Applicant: SERVIER LAB

Inventor： METH-COHN OTTO ,  YU CHU-YI ,  LESTAGE PIERRE ,  LEBRUN MARIE-CECILE ,  CAIGNARD DANIEL-HENRI ,  RENARD PIERRE

IPC: C07D211/00 ,  A61K31/435 ,  A61K31/44 ,  A61K31/4402 ,  A61K31/4418 ,  A61K31/4425 ,  A61K31/4439 ,  A61K31/445 ,  A61K31/4458 ,  A61K31/451 ,  A61K31/452 ,  A61K31/5377 ,  A61P25/00 ,  A61P25/02 ,  A61P25/04 ,  A61P25/16 ,  A61P25/28 ,  B01J23/42 ,  C07B61/00 ,  C07D211/22 ,  C07D211/32 ,  C07D213/30 ,  C07D213/36 ,  C07D213/38 ,  C07D213/50 ,  C07D401/06

Abstract: PROBLEM TO BE SOLVED: To obtain a compound capable of resisting dysgnosia with aging and ameliorating a recognition process, having analgesic characteristics. SOLUTION: This compound is represented by formula (I) [A is pyridine, or the like; R2 is hydrogen atom, or the like; R3 is hydroxy group, or the like; R4 is phenyl group, or the like; R1 is hydrogen atom, or the like; R5 is a five- or six-membered ring which may contain a nitrogen atom combined with the ring A and another hetero atom selected from sulfur, oxygen and nitrogen; R6 is hydrogen atom, or the like], its enantiomer, a diastereoisomer, pharmacologically acceptable acid, base or their addition salts. The method for producing the compound is provided. The medicine composition comprises the compound.

公开(公告)号：WO2004043956A8

公开(公告)日：2005-06-09

申请号：PCT/FR0303274

申请日：2003-11-04

Applicant: SERVIER LAB ,  RAULT SYLVAIN ,  LANCELOT JEAN-CHARLES ,  KOPP MARINA ,  CAIGNARD DANIEL-HENRI ,  PFEIFFER BRUNO ,  RENARD PIERRE

Inventor： RAULT SYLVAIN ,  LANCELOT JEAN-CHARLES ,  KOPP MARINA ,  CAIGNARD DANIEL-HENRI ,  PFEIFFER BRUNO ,  RENARD PIERRE

IPC: A61P3/04 ,  A61P3/10 ,  A61P9/10 ,  A61P9/12 ,  A61P19/02 ,  A61P35/00 ,  C07D471/04 ,  A61K31/505

CPC classification number: C07D471/04

Abstract: Compounds of formula (I), where: R1, R2, R3, R4 are as defined in the description, the enantiomers, diastereomers, tautomers and addition salts thereof with a pharmaceutically-acceptable acid or base. Said compounds have kinase modulating properties and are useful in the treatment of cancer, diabetes, obesity etc.

Abstract translation: 式（I）化合物，其中：R 1，R 2，R 3，R 4如说明书中所定义，其对映异构体，非对映异构体，互变异构体及其药学上可接受的酸或碱的加成盐。 所述化合物具有激酶调节性质，可用于治疗癌症，糖尿病，肥胖等。

公开(公告)号：WO0200638A2

公开(公告)日：2002-01-03

申请号：PCT/IB0101535

申请日：2001-06-27

Applicant: INST MATERIA MEDICA ,  SERVIER LAB ,  GUO ZONGRU ,  CHU FENGMING ,  ZHANG JUNTIAN ,  YANG GUANGZHONG ,  XU BAILING ,  NIU XINYI ,  REN ZHIHONG ,  LESTAGE PIERRE ,  RENARD PIERRE

Inventor： GUO ZONGRU ,  CHU FENGMING ,  ZHANG JUNTIAN ,  YANG GUANGZHONG ,  XU BAILING ,  NIU XINYI ,  REN ZHIHONG ,  LESTAGE PIERRE ,  RENARD PIERRE

IPC: C07D307/88 ,  A61K31/34 ,  A61K31/365 ,  A61P9/10 ,  A61P25/00 ,  A61P25/08 ,  A61P25/16 ,  A61P25/28 ,  C07D239/42 ,  C07D471/04 ,  C07D487/04 ,  C07D307/00

CPC classification number: C07D239/42 ,  C07D471/04 ,  C07D487/04

Abstract: The invention relates to compounds of formula (I): wherein R represents an alkyl or ureido group, R represents an alkyl group or a hydrogen atom, or R and R together form a 5- or 6-membered ring, R represents a group CN, NO2, NRaR'a, NRaSO2,R'aCZR or CZNRaR'a, R represents a hydrogen atom or a group R .

Abstract translation: 本发明涉及式（I）化合物：其中R 1表示烷基或脲基，R 2表示烷基或氢原子，或R 1和R 2一起形成5 - 或6-元环，R 3表示CN，NO 2，NR a R aa，NR a SO 2，R'CZR 5或CZNR a R aa，R 4表示氢原子或基团R 3， 。

公开(公告)号：WO0200638A8

公开(公告)日：2003-08-28

申请号：PCT/IB0101535

申请日：2001-06-27

Applicant: INST MATERIA MEDICA ,  SERVIER LAB ,  GUO ZONGRU ,  CHU FENGMING ,  ZHANG JUNTIAN ,  YANG GUANGZHONG ,  XU BAILING ,  NIU XINYI ,  REN ZHIHONG ,  LESTAGE PIERRE ,  RENARD PIERRE

Inventor： GUO ZONGRU ,  CHU FENGMING ,  ZHANG JUNTIAN ,  YANG GUANGZHONG ,  XU BAILING ,  NIU XINYI ,  REN ZHIHONG ,  LESTAGE PIERRE ,  RENARD PIERRE

IPC: C07D307/88 ,  A61K31/34 ,  A61K31/365 ,  A61P9/10 ,  A61P25/00 ,  A61P25/08 ,  A61P25/16 ,  A61P25/28 ,  C07D239/42 ,  C07D471/04 ,  C07D487/04

CPC classification number: C07D239/42 ,  C07D471/04 ,  C07D487/04

Abstract: The invention relates to compounds of formula (I): wherein R represents an alkyl or ureido group, R represents an alkyl group or a hydrogen atom, or R and R together form a 5- or 6-membered ring, R represents a group CN, NO2, NRaR'a, NRaSO2,R'aCZR or CZNRaR'a, R represents a hydrogen atom or a group R .

Abstract translation: 本发明涉及式（I）化合物：其中R 1表示烷基或脲基，R 2表示烷基或氢原子，或R 1和R 2一起形成5 - 或6-元环，R 3表示CN，NO 2，NR a R aa，NR a SO 2，R'CZR 5或CZNR a R aa，R 4表示氢原子或基团R 3， 。

公开(公告)号：WO02094840A2

公开(公告)日：2002-11-28

申请号：PCT/FR0201716

申请日：2002-05-22

Applicant: SERVIER LAB ,  HUSSON HENRI-PHILIPPE ,  GIORGI-RENAULT SYLVIANE ,  DESBENE STEPHANIE ,  HICKMAN JOHN ,  PIERRE ALAIN ,  KRAUS-BERTHIER LAURENCE ,  PFEIFFER BRUNO ,  RENARD PIERRE

Inventor： HUSSON HENRI-PHILIPPE ,  GIORGI-RENAULT SYLVIANE ,  DESBENE STEPHANIE ,  HICKMAN JOHN ,  PIERRE ALAIN ,  KRAUS-BERTHIER LAURENCE ,  PFEIFFER BRUNO ,  RENARD PIERRE

IPC: A61K31/4741 ,  A61K31/4743 ,  A61K31/4745 ,  A61K31/661 ,  A61P35/00 ,  C07D471/04 ,  C07D491/04 ,  C07D491/048 ,  C07D491/056 ,  C07D491/14 ,  C07D497/04 ,  C07F9/60 ,  C07F9/6561

CPC classification number: C07D491/04 ,  C07D491/14 ,  C07F9/6561

Abstract: The invention concerns a compound of formula (I), wherein: (a) represents a single or double bond; (b) represents a cycle selected among (i), (ii), (iii), (iv) and (v); R9a, R9b, R9c, X and Y are such as defined in the description; R1 represents a group selected among hydrogen, aryl, heteroaryl, cycloalkyl, alkyl optionally substituted, and COR11, wherein R11 is such as defined in the description; R2 to R8 represent each a group selected among hydrogen, halogen, hydroxy, polyhalogenoalkyl, nitro, alkyl optionally substituted, amino optionally substituted, alkoxy optionally substituted, -OPO(OH)2 and (II), wherein m represents an integer such that 1

Abstract translation: 本发明涉及式（I）化合物，其中：（a）表示单键或双键; （b）表示选自（i），（ii），（iii），（iv）和（v）中的循环; R9a，R9b，R9c，X和Y如描述中所定义; R 1表示选自氢，芳基，杂芳基，环烷基，任选取代的烷基和COR 11中的基团，其中R 11如说明书中所定义; R 2至R 8表示选自氢，卤素，羟基，多卤代烷基，硝基，任选取代的烷基，任选取代的氨基，任选取代的烷氧基，-OPO（OH）2和（II）中的基团，其中m表示1 R 3或具有R 4的R 3或具有R 5的R 4一起与含有任选含有1或2个杂原子并任选取代的单环或双环基团的碳原子一起形成; R 16表示氢原子或烷基; （c）表示芳基，杂芳基或芳基烷基; 以及其光学异构体，其与药学上可接受的酸或碱的加成盐以及其水合物和溶剂合物。 本发明可用于制备药物。

公开(公告)号：EG24967A

公开(公告)日：2011-03-13

申请号：EG2004070320

申请日：2004-07-28

Applicant: SERVIER LAB

Inventor： LECLERC VERONIQUE ,  PAILLOUX SYLVIE ,  CARATO PASCAL ,  INTROVIGNE CARINE ,  LEBEGUE NICOLAS ,  BERTHELOT PASCAL ,  DACQUET CATHERINE ,  BOUTIN JEAN ALBERT ,  CAIGNARD DANIEL HENRI ,  RENARD PIERRE

IPC: C07D235/26 ,  A61K31/426 ,  A61K31/427 ,  A61P1/04 ,  A61P1/18 ,  A61P3/06 ,  A61P3/10 ,  A61P9/00 ,  A61P9/10 ,  A61P13/04 ,  A61P13/12 ,  A61P15/00 ,  A61P17/06 ,  A61P19/10 ,  A61P21/04 ,  A61P25/28 ,  A61P27/02 ,  A61P35/00 ,  C07D235/12 ,  C07D277/68 ,  C07D417/10 ,  C07D417/12

Abstract: Benzoxazole, benzothiazole or indole oxime derivatives (I) (including analogs with the benzo ring replaced by pyridine, pyrazine, pyrimidine or pyridazine) are new. Benzoxazole, benzothiazole or indole oxime derivatives of formula (I) (including analogs with the benzo ring replaced by pyridine, pyrazine, pyrimidine or pyridazine), and their enantiomers, diastereomers and salts are new. [Image] X : O, S, CH 2 or CHR' 2>; R 1>, R 2>H, alkyl, aryl, aralkyl, aryloxy, aralkoxy, alkoxy, OH, NH 2 or mono- or dialkylamino; or R 1> + R 2>=O, =S or =NH; R' 2>group forming an additional bond with R 2>; A : 1-6C alkylene (optionally having one CH 2 replaced by O, S, NRa', phenylene or naphthylene); Ra' : H or alkyl; R 3>, R 4>H, halo, R, OR or NRR'; or R 3> + R 4>group forming an ortho-fused 5- or 6-membered ring (optionally containing an O, S or N heteroatom); R, R', R 5>, R 6>H, alkyl, alkenyl, alkynyl, aryl, aralkyl, aralkenyl, aralkynyl, heteroaryl, heteroaralkyl, heteroaralkenyl, heteroaralkynyl, cycloalkyl, cycloalkylalkyl or polyhaloalkyl; D : benzene ring (in which case X is other than CHR' 2>); or a pyridine, pyrazine, pyrimidine or pyridazine ring; B : alkyl or alkenyl, both substituted by -CHR 7>R 8> or by R 9>; or -CHR 7>R 8> or R 9>; R 7>-C(Z)OR, -C(Z)NRR', -N(R)C(Z)R' or -N(R)C(Z)OR'; Z : O or S; R 8>aryl, aralkyl, heteroaryl, heteroaralkyl, CN, tetrazole, OR, NRR', -N(R)C(Z)R' or -N(R)C(Z)OR'; R 9>CN, tetrazole, -N(R)C(Z)R', -N(R)C(Z)OR' or -O(CH 2) n-CR 1> 0>R 1> 1>-COOR; n : 0-6; R 1> 0>, R 1> 1>H or alkyl, but not both H; aryl moieties : phenyl, naphthyl or biphenyl (all optionally partially hydrogenated and optionally substituted by 1-3 alkyl, polyhaloalkyl, alkoxy, OH, COOH, CHO, NRaRb, ester, amido, NO 2, CN or halo groups); heteroaryl moieties : 5-10 membered mono- or bicyclic aryl (where one ring is optionally partially hydrogenated in the case of bicyclic systems) containing 1-3 O, S and/or N heteroatom(s) and optionally substituted as for aryl; Rb, Rc : H, alkyl, aryl or heteroaryl; the oxime group -C(R 6>)=NOR 5> has E- or Z-configuration; alkyl moieties have 1-6C, alkenyl or alkynyl moieties 2-6C and cycloalkyl moieties 3-8C. Independent claims are included for: (1) preparation method of (I); and (2) new ketone intermediates of formula (V). [Image] ACTIVITY : Antidiabetic; Antilipemic; Cardiant; Nephrotropic; Ophthalmological; Antipsoriatic; Gynecological; Nootropic; Osteopathic; Antiinflammatory; Antiarteriosclerotic; Anorectic; Cytostatic. In tests in ob/ob mice, oral administration of 10 mg/kg of methyl 3-(4-(2-(6-((methoxyimino)-(phenyl)-methyl)-2-oxo-1,3-benzothiazol-3(2H)-yl)-ethoxy)-phenyl)-2-(2,2,2-trifluoroethoxy)-propanoate (Ia) twice per day for 4 days reduced blood sugar levels by 51% and reduced the weight gain by 80% in comparison with controls, whereas analogous administration of rosiglitazone reduced blood sugar levels by 61% but increased the weight gain by 33% in comparison with controls. MECHANISM OF ACTION : Aldose Reductase Inhibitor; Angiogenesis Inhibitor.

公开(公告)号：NO327257B1

公开(公告)日：2009-05-25

申请号：NO20043188

申请日：2004-07-27

Applicant: SERVIER LAB

Inventor： LECLERC VERONIQUE ,  RENARD PIERRE ,  CAIGNARD DANIEL-HENRI ,  CARATO PASCAL ,  PAILLOUX SYLVIE ,  INTROVIGNE CARINE ,  LEBEGUE NICOLAS ,  BERTHELOT PASCAL ,  DACQUET CATHRINE ,  BOUTIN JEAN ALBERT

IPC: C07D235/26 ,  C07D277/68 ,  A61K31/426 ,  A61K31/427 ,  A61P1/04 ,  A61P1/18 ,  A61P3/06 ,  A61P3/10 ,  A61P9/00 ,  A61P9/10 ,  A61P13/04 ,  A61P13/12 ,  A61P15/00 ,  A61P17/06 ,  A61P19/10 ,  A61P21/04 ,  A61P25/28 ,  A61P27/02 ,  A61P35/00 ,  C07D235/12 ,  C07D417/10 ,  C07D417/12

Abstract: Benzoxazole, benzothiazole or indole oxime derivatives (I) (including analogs with the benzo ring replaced by pyridine, pyrazine, pyrimidine or pyridazine) are new. Benzoxazole, benzothiazole or indole oxime derivatives of formula (I) (including analogs with the benzo ring replaced by pyridine, pyrazine, pyrimidine or pyridazine), and their enantiomers, diastereomers and salts are new. [Image] X : O, S, CH 2 or CHR' 2>; R 1>, R 2>H, alkyl, aryl, aralkyl, aryloxy, aralkoxy, alkoxy, OH, NH 2 or mono- or dialkylamino; or R 1> + R 2>=O, =S or =NH; R' 2>group forming an additional bond with R 2>; A : 1-6C alkylene (optionally having one CH 2 replaced by O, S, NRa', phenylene or naphthylene); Ra' : H or alkyl; R 3>, R 4>H, halo, R, OR or NRR'; or R 3> + R 4>group forming an ortho-fused 5- or 6-membered ring (optionally containing an O, S or N heteroatom); R, R', R 5>, R 6>H, alkyl, alkenyl, alkynyl, aryl, aralkyl, aralkenyl, aralkynyl, heteroaryl, heteroaralkyl, heteroaralkenyl, heteroaralkynyl, cycloalkyl, cycloalkylalkyl or polyhaloalkyl; D : benzene ring (in which case X is other than CHR' 2>); or a pyridine, pyrazine, pyrimidine or pyridazine ring; B : alkyl or alkenyl, both substituted by -CHR 7>R 8> or by R 9>; or -CHR 7>R 8> or R 9>; R 7>-C(Z)OR, -C(Z)NRR', -N(R)C(Z)R' or -N(R)C(Z)OR'; Z : O or S; R 8>aryl, aralkyl, heteroaryl, heteroaralkyl, CN, tetrazole, OR, NRR', -N(R)C(Z)R' or -N(R)C(Z)OR'; R 9>CN, tetrazole, -N(R)C(Z)R', -N(R)C(Z)OR' or -O(CH 2) n-CR 1> 0>R 1> 1>-COOR; n : 0-6; R 1> 0>, R 1> 1>H or alkyl, but not both H; aryl moieties : phenyl, naphthyl or biphenyl (all optionally partially hydrogenated and optionally substituted by 1-3 alkyl, polyhaloalkyl, alkoxy, OH, COOH, CHO, NRaRb, ester, amido, NO 2, CN or halo groups); heteroaryl moieties : 5-10 membered mono- or bicyclic aryl (where one ring is optionally partially hydrogenated in the case of bicyclic systems) containing 1-3 O, S and/or N heteroatom(s) and optionally substituted as for aryl; Rb, Rc : H, alkyl, aryl or heteroaryl; the oxime group -C(R 6>)=NOR 5> has E- or Z-configuration; alkyl moieties have 1-6C, alkenyl or alkynyl moieties 2-6C and cycloalkyl moieties 3-8C. Independent claims are included for: (1) preparation method of (I); and (2) new ketone intermediates of formula (V). [Image] ACTIVITY : Antidiabetic; Antilipemic; Cardiant; Nephrotropic; Ophthalmological; Antipsoriatic; Gynecological; Nootropic; Osteopathic; Antiinflammatory; Antiarteriosclerotic; Anorectic; Cytostatic. In tests in ob/ob mice, oral administration of 10 mg/kg of methyl 3-(4-(2-(6-((methoxyimino)-(phenyl)-methyl)-2-oxo-1,3-benzothiazol-3(2H)-yl)-ethoxy)-phenyl)-2-(2,2,2-trifluoroethoxy)-propanoate (Ia) twice per day for 4 days reduced blood sugar levels by 51% and reduced the weight gain by 80% in comparison with controls, whereas analogous administration of rosiglitazone reduced blood sugar levels by 61% but increased the weight gain by 33% in comparison with controls. MECHANISM OF ACTION : Aldose Reductase Inhibitor; Angiogenesis Inhibitor.