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首页> 外文期刊>Journal of Medicinal Chemistry >Human Glucagon Receptor Antagonists with Thiazole Cores. A Novel Series with Superior Pharmacokinetic Properties
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Human Glucagon Receptor Antagonists with Thiazole Cores. A Novel Series with Superior Pharmacokinetic Properties

机译:具有噻唑核心的人胰高血糖素受体拮抗剂。具有优异药代动力学特性的新型系列

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摘要

The aim of the work presented here was to design and synthesize potent human glucagon receptor antagonists with improved pharmacokinetic (PK) properties for development of pharmaceuticals for the treatment of type 2 diabetes. We describe the preparation of compounds with cyclic cores (5-aminothiazoles), their binding affinities for the human glucagon and GIP receptors, as well as affinities for rat, mouse, pig, dog, and monkey glucagon receptors. Generally, the compounds had slightly less glucagon receptor affinity compared to compounds of the previous series, but this was compensated for by much improved PK profiles in both rats and dogs with high oral bioavailabilities and sustained high plasma exposures. The compounds generally showed species selectivity for glucagon receptor binding with poor affinities for the rat, mouse, rabbit, and pig receptors. However, dog and monkey glucagon receptor affinities seem to reflect the human situation. One compound of this series, 18, was tested intravenously in an anesthetized glucagon-challenged monkey model of hyperglucagonaemia and hyperglycaemia and was shown dose-dependently to decrease glycaemia. Further, high plasma exposures and a long plasma half-life (5.2 h) were obtained.
机译:本文提出的工作目的是设计和合成具有改善的药代动力学(PK)性质的有效人胰高血糖素受体拮抗剂,以开发用于治疗2型糖尿病的药物。我们描述了具有环核(5-氨基噻唑)的化合物的制备,它们对人胰高血糖素和GIP受体的结合亲和力以及对大鼠,小鼠,猪,狗和猴胰高血糖素受体的亲和力。通常,与先前系列的化合物相比,该化合物的胰高血糖素受体亲和力略低,但这可以通过口服生物利用度高和血浆暴露持续高的大鼠和狗的PK分布大大改善来弥补。这些化合物通常对胰高血糖素受体结合表现出物种选择性,而对大鼠,小鼠,兔和猪受体的亲和力却很差。但是,狗和猴子的胰高血糖素受体亲和力似乎反映了人类的处境。在麻醉的胰高血糖素血症和高血糖症的猴子模型中,静脉内测试了该系列化合物之一18,并显示出剂量依赖性地降低了血糖。此外,获得了较高的血浆暴露量和较长的血浆半衰期(5.2小时)。

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