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Exchange protein directly activated by cyclic AMP isoform 2 is not a direct target of sulfonylurea drugs.

机译:由环AMP亚型2直接激活的交换蛋白不是磺脲类药物的直接靶标。

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摘要

It has been reported by Zhang et al. that antidiabetic sulfonylurea drugs promote insulin secretion by directly binding to exchange protein directly activated by cyclic AMP isoform 2 (Epac2) and activating its down-stream effector Rap1. However, a critical link for an unambiguous validation of a direct interaction between Epac2 and sulfonylurea using purified individual components is missing. Our in vitro analyses using purified full-length Epac2 and Rap1 suggest that sulfonylureas are not able to directly bind to Epac2, nor are they capable of triggering Epac2-dependent Rap1 activation.
机译:Zhang等报道,抗糖尿病磺酰脲类药物通过直接结合由环AMP亚型2(Epac2)直接激活的交换蛋白并激活其下游效应子Rap1来促进胰岛素分泌。然而,使用纯化的单个组分明确验证 Epac2 和磺酰脲类药物之间直接相互作用的关键环节缺失。我们使用纯化的全长 Epac2 和 Rap1 进行的体外分析表明,磺脲类药物不能直接与 Epac2 结合,也不能触发 Epac2 依赖性 Rap1 激活。

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