THE SYNTHESIS OF NOVEL GABA UPTAKE INHIBITORS .1. ELUCIDATION OF THE STRUCTURE-ACTIVITY STUDIES LEADING TO THE CHOICE OF (R)-1-[4,4-BIS(3-METHYL-2-THIENYL)-3-BUTENYL]-3-PIPERIDINECARBOXYLIC ACID (TIAGABINE) AS AN ANTICONVULSANT DRUG CANDIDATE

被引：139

作者：

ANDERSEN, KE ^{[1
]}

BRAESTRUP, C ^{[1
]}

GRONWALD, FC ^{[1
]}

JORGENSEN, AS ^{[1
]}

NIELSEN, EB ^{[1
]}

SONNEWALD, U ^{[1
]}

SORENSEN, PO ^{[1
]}

SUZDAK, PD ^{[1
]}

KNUTSEN, LJS ^{[1
]}

机构：

[1] NOVO NORDISK AS,DIV PHARMACEUT,NOVO NORDISK PK,DK-2760 MALOV,DENMARK

来源：

JOURNAL OF MEDICINAL CHEMISTRY | 1993年 / 36卷 / 12期

关键词：

D O I：

10.1021/jm00064a005

中图分类号：

R914 [药物化学];

学科分类号：

100701 ;

摘要：

A series of different synthetic approaches to novel GABA uptake inhibitors are described, leading to examples which are derivatives of nipecotic acid and guvacine, substituted at nitrogen by 4,4-diaryl-3-butenyl or 2-(diphenylmethoxy)ethyl moieties. The in vitro value for inhibition of [H-3]-GABA uptake in rat synaptosomes was determined for each compound. It was found that the most potent examples are those having a substituent in an ''ortho'' position in one or both aromatic/heteroaromatic groups. The majority of the compounds described are structurally related to tiagabine, (R)-1-[4,4-bis(3-methyl-2-thienyl)-3-butenyl]-3-piperidinecarboxylic acid hydrochloride (NNC 05-0328) and some of the reasoning behind the selection of this compound as a drug candidate is summarized.

引用

页码：1716 / 1725

页数：10

共 67 条

[1]

AKKERMAN AM, 1951, RECL TRAV CHIM PAY B, V70, P899

[2] ORALLY ACTIVE AND POTENT INHIBITORS OF GAMMA-AMINOBUTYRIC ACID UPTAKE [J].

ALI, FE ;

BONDINELL, WE ;

DANDRIDGE, PA ;

FRAZEE, JS ;

GARVEY, E ;

GIRARD, GR ;

KAISER, C ;

KU, TW ;

LAFFERTY, JJ ;

MOONSAMMY, GI ;

OH, HJ ;

RUSH, JA ;

SETLER, PE ;

STRINGER, OD ;

VENSLAVSKY, JW ;

VOLPE, BW ;

YUNGER, LM ;

ZIRKLE, CL .

JOURNAL OF MEDICINAL CHEMISTRY, 1985, 28 (05) :653-660

[3] THE REACTION OF TRIMETHYL CHLOROSILANE WITH ALPHA-CYCLOPROPANIC ALCOHOLS IN THE PRESENCE OR IN THE ABSENCE OF LITHIUM HALOGENIDES [J].

BALME, G ;

FOURNET, G ;

GORE, J .

TETRAHEDRON LETTERS, 1986, 27 (17) :1907-1908

[4]

BETTONI G, 1972, GAZZ CHIM ITAL, V102, P189

[5] SYNTHESIS AND METABOLIC PROFILE OF CI-966 - A POTENT, ORALLY-ACTIVE INHIBITOR OF GABA UPTAKE [J].

BJORGE, S ;

BLACK, A ;

BOCKBRADER, H ;

CHANG, T ;

GREGOR, VE ;

LOBBESTAEL, SJ ;

NUGIEL, D ;

PAVIA, MR ;

RADULOVIC, L ;

WOOLF, T .

DRUG DEVELOPMENT RESEARCH, 1990, 21 (03) :189-193

[6]

Bodor N., 1983, PHARMACOL THERAPEUT, V19, P337

[7] GABA TRANSPORTER PROTEIN CLONED FROM RAT-BRAIN [J].

BOWERY, NG .

TRENDS IN PHARMACOLOGICAL SCIENCES, 1990, 11 (11) :435-437

[8] (R)-N-[4,4-BIS(3-METHYL-2-THIENYL)BUT-3-EN-1-YL]NIPECOTIC ACID BINDS WITH HIGH-AFFINITY TO THE BRAIN GAMMA-AMINOBUTYRIC ACID UPTAKE CARRIER [J].

BRAESTRUP, C ;

NIELSEN, EB ;

SONNEWALD, U ;

KNUTSEN, LJS ;

ANDERSEN, KE ;

JANSEN, JA ;

FREDERIKSEN, K ;

ANDERSEN, PH ;

MORTENSEN, A ;

SUZDAK, PD .

JOURNAL OF NEUROCHEMISTRY, 1990, 54 (02) :639-647

[9]

BRAESTRUP C, 1987, INT C SER EXCERPTA M, V750, P125

[10]

CAUSTLAND DJ, 1974, J MED CHEM, V17, P993

← 1 2 3 4 5 6 7 →