Potent benzimidazole sulfonamide protein tyrosine phosphatase 1B inhibitors containing the Heterocyclic (S)-isothiazolidinone phosphotyrosine mimetic

被引:96
作者
Combs, Andrew P.
Zhu, Wenyu
Crawley, Matthew L.
Glass, Brian
Polam, Padmaja
Sparks, Richard B.
Modi, Dilip
Takvorian, Amy
McLaughlin, Erin
Yue, Eddy W.
Wasserman, Zelda
Bower, Michael
Wei, Min
Rupar, Mark
Ala, Paul J.
Reid, Brian M.
Ellis, Dawn
Gonneville, Lucie
Emm, Thomas
Taylor, Nancy
Yeleswaram, Swamy
Li, Yanlong
Wynn, Richard
Burn, Timothy C.
Hollis, Gregory
Liu, Phillip C. C.
Metcalf, Brian
机构
[1] Incyte Corp, Discovery Chem, Wilmington, DE 19880 USA
[2] Incyte Corp, Appl Technol, Wilmington, DE 19880 USA
[3] Incyte Corp, Drug Metab, Expt Stn, Wilmington, DE 19880 USA
关键词
D O I
10.1021/jm0600904
中图分类号
R914 [药物化学];
学科分类号
100701 ;
摘要
Potent nonpeptidic benzimidazole sulfonamide inhibitors of protein tyrosine phosphatase 1B (PTP1B) were derived from the optimization of a tripeptide containing the novel (S)-isothiazolidinone ((S)-IZD) phosphotyrosine ( pTyr) mimetic. An X-ray cocrystal structure of inhibitor 46/PTP1B at 1.8 angstrom resolution demonstrated that the benzimidazole sulfonamides form a bidentate H bond to Asp48 as designed, although the aryl group of the sulfonamide unexpectedly interacts intramolecularly in a pi-stacking manner with the benzimidazole. The ortho substitution to the (S)-IZD on the aryl ring afforded low nanomolar enzyme inhibitors of PTP1B that also displayed low caco-2 permeability and cellular activity in an insulin receptor (IR) phosphorylation assay and an Akt phosphorylation assay. The design, synthesis, and SAR of this novel series of benzimidazole sulfonamide containing (S)-IZD inhibitors of PTP1B are presented herein.
引用
收藏
页码:3774 / 3789
页数:16
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