Design and synthesis of thrombin inhibitors: Analogues of MD-805 with reduced stereogenicity and improved potency

被引:34
作者
Brundish, D
Bull, A
Donovan, V
Fullerton, JD
Garman, SM
Hayler, JF
Janus, D
Kane, PD
McDonnell, M
Smith, GP
Wakeford, R
Walker, CV
Howarth, G
Hoyle, W
Allen, MC
Ambler, J
Butler, K
Talbot, MD
机构
[1] Novartis Horsham, Res Ctr, Dept Chem, Horsham RH12 5AB, W Sussex, England
[2] Novartis Horsham, Res Ctr, Dept Biol, Horsham RH12 5AB, W Sussex, England
[3] Novartis Horsham, Res Ctr, Drug Discovery Support, Horsham RH12 5AB, W Sussex, England
[4] Ciba Cent Res Labs, Macclesfield SK10 2NX, Cheshire, England
关键词
D O I
10.1021/jm9811209
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
Mitsubishi's MD-805, a potent and selective inhibitor of thrombin which contains four stereogenic centers, has been the starting point for an optimization program. A systematic synthetic study resulted in thrombin inhibit;ors achiral at P2 and P3 but with a 10-fold increase in potency over the original lead. A number of 4-substituted piperidines were synthesized and examined as replacements for 2-carboxy-4-methylpiperidine at P2; 4-fluoroethylpiperidine (FEP) among others provided inhibitors (e.g. 45g) of increased potency. An enantioselective route was developed to 3(R)-methyl-1,2,3,4-tetrahydroquinolinesulfonyl chloride. Inhibitors containing this enantiomerically pure P3 (42d) had similar potency to the racemic material and provided support, with modeling studies, for the preparation of the gem 3,3-disubstituted compounds. A series of inhibitors containing the novel 3,3-dimethyl-1,2,3,4-tetrahydroquinolinesulfonyl (DMTHQS) P3 (Table 5) were synthesized and showed a similar activity profile as the monomethyl series. The combination of P3-DMTHQS, PB-FEP, and P1-arginine (45g) had a K-i of 6 nM (MD-805 K-i = 85 nM). In animal models of both venous and arterial thrombosis, one inhibitor (42e) was shown to produce a dose-dependent inhibition of thrombus formation that in some situations was superior to that of MD-805.
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页码:4584 / 4603
页数:20
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