PDE-10A inhibitors as insulin secretagogues

被引：38

作者：

Cantin, Louis-David ^{[1
]}

Magnuson, Steven

Gunn, David

Barucci, Nicole

Breuhaus, Marina

Bullock, William H.

Burke, Jennifer

Claus, Thomas H.

Daly, Michelle

DeCarr, Lynn

Gore-Willse, Ann

Hoover-Litty, Helana

Kumarasinghe, Ellalahewage S.

Li, Yaxin

Liang, Sidney X.

Livingston, James N.

Lowinger, Timothy

MacDougall, Margit

Ogutu, Herbert O.

Olague, Alan

Ott-Morgan, Ronda

Schoenleber, Robert W.

Tersteegen, Adrian

Wickens, Philip

Zhang, Zhonghua

Zhu, Jian

Zhu, Lei

Sweet, Laurel J.

机构：

[1] Bayer Pharmaceut Corp, Dept Chem Res, West Haven, CT 06516 USA

[2] Bayer Pharmaceut Corp, Dept Metab Disorders Res, West Haven, CT 06516 USA

[3] Bayer Pharmaceut Corp, Dept Res Technol, West Haven, CT 06516 USA

[4] Bayer HealthCare, Dept Cardiovasc Res & Screening, Wuppertal, Germany

来源：

BIOORGANIC & MEDICINAL CHEMISTRY LETTERS | 2007年 / 17卷 / 10期

关键词：

PDE-10A inhibition; insulin secretagogue; quinoline; type; 2; diabetes;

D O I：

10.1016/j.bmcl.2007.02.061

中图分类号：

R914 [药物化学];

学科分类号：

100701 ;

摘要：

Modulation of cAMP levels has been linked to insulin secretion in preclinical animal models and in humans. The high expression of PDE-10A in pancreatic islets suggested that inhibition of this enzyme may provide the necessary modulation to elicit increased insulin secretion. Using an HTS approach, we have identified quinoline-based PDE-10A inhibitors as insulin secretagogues in vitro. Optimized compounds were evaluated in vivo where improvements in glucose tolerance and increases in insulin secretion were measured. (c) 2007 Elsevier Ltd. All rights reserved.

引用

页码：2869 / 2873

页数：5

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