Sanofi-Aventis Deutschland GmbH, R&D, Diabetes Division, Industriepark Hoechst, Building G 878, D-65926 Frankfurt am Main, Germany.
J Med Chem. 2010 Dec 23;53(24):8679-87. doi: 10.1021/jm101179e. Epub 2010 Nov 17.
Acetyl CoA carboxylase isoforms 1 and 2 (ACC1/2) are key enzymes of fat utilization and their inhibition is considered to improve aspects of the metabolic syndrome. To identify pharmacological inhibitors of ACC1/2, a high throughput screen was performed which resulted in the identification of the lead compound 3 ( Gargazanli , G. ; Lardenois , P. ; Frost , J. ; George , P. Patent WO9855474 A1, 1998 ) as a moderate selective ACC2 inhibitor. Optimization of 3 led to 4m ( Zoller , G. ; Schmoll , D. ; Mueller , M. ; Haschke , G. ; Focken , I. Patent WO2010003624 A2, 2010 ) as a submicromolar dual ACC1/2 inhibitor of the rat and human isoforms. 4m possessed favorable pharmacokinetic parameters. This compound stimulated fat oxidation in vivo and reduced plasma triglyceride levels in a rodent model after subchronic administration. 4m is a suitable tool compound for the elucidation of the pharmacological potential of ACC1/2 inhibition.
乙酰辅酶 A 羧化酶同工酶 1 和 2(ACC1/2)是脂肪利用的关键酶,其抑制被认为可以改善代谢综合征的某些方面。为了鉴定 ACC1/2 的药理学抑制剂,进行了高通量筛选,从而鉴定出先导化合物 3( Gargazanli,G.;Lardenois,P.;Frost,J.;George,P.专利 WO9855474 A1,1998 年)作为中度选择性 ACC2 抑制剂。对 3 的优化导致了 4m(Zoller,G.;Schmoll,D.;Mueller,M.;Haschke,G.;Focken,I.专利 WO2010003624 A2,2010 年)作为大鼠和人同工型的亚微摩尔双重 ACC1/2 抑制剂。4m 具有良好的药代动力学参数。该化合物在体内刺激脂肪氧化,并在亚慢性给药后降低啮齿动物模型中的血浆甘油三酯水平。4m 是阐明 ACC1/2 抑制的药理学潜力的合适工具化合物。
