化学
生物利用度
药代动力学
嘧啶
代谢物
立体化学
活性代谢物
药理学
组合化学
生物化学
医学
作者
James S. Scott,Adrian L. Gill,Linda Godfrey,Sam D. Groombridge,Amanda Rees,John Revill,Paul N. Schofield,Pernilla Sörme,Andrew Stocker,John G. Swales,Paul R. O. Whittamore
标识
DOI:10.1016/j.bmcl.2012.08.070
摘要
11β-HSD1 is increasingly seen as an attractive target for the treatment of type II diabetes and other elements of the metabolic syndrome. In this program of work we describe how a series of neutral 2-thioalkyl-pyridine 11β-HSD1 inhibitors were optimized in terms of their pharmacokinetic properties to give compounds with excellent bioavailability in both rat and dog through a core change to pyrimidine. A potential reactive metabolite issue with 4-thioalkyl-pyrimidines was circumvented by a switch from sulfur to carbon substitution.
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