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Chemical Probe Identification Platform for Orphan GPCRs Using Focused Compound Screening: GPR39 as a Case Example

机译:用于孤儿GPCR的化学探针鉴定平台,使用重点化合物筛选:以GPR39为例

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摘要

Orphan G protein-coupled receptors (oGPCRs) are a class of integral membrane proteins for which endogenous ligands or transmitters have not yet been discovered. Transgenic animal technologies have uncovered potential roles for many of these oGPCRs, providing new targets for the treatment of various diseases. Understanding signaling pathways of oGPCRs and validating these receptors as potential drug targets requires the identification of chemical probe compounds to be used in place of endogenous ligands to interrogate these receptors. A novel chemical probe identification platform was created in which GPCR-focused libraries were screened against sets of oGPCR targets, with a goal of discovering fit-for-purpose chemical probes for the more druggable members of the set. Application of the platform to a set of oGPCRs resulted in the discovery of the first reported small molecule agonists for GPR39, a receptor implicated in the regulation of insulin secretion and preservation of beta cells in the pancreas. Compound 1 stimulated intracellular calcium mobilization in recombinant and native cells in a GPR39-specific manner but did not potentiate glucosestimulated insulin secretion in human islet preparations.
机译:孤儿G蛋白偶联受体(oGPCR)是一类完整的膜蛋白,尚未发现其内源性配体或递质。转基因动物技术已经发现了许多这类oGPCR的潜在作用,为治疗各种疾病提供了新的靶点。了解oGPCR的信号传导途径并验证这些受体作为潜在的药物靶标,需要鉴定化学探针化合物来代替内源性配体来询问这些受体。创建了一个新的化学探针鉴定平台,在该平台中针对oGPCR靶标集筛选了以GPCR为重点的文库,目的是为该组中更易吸毒的成员发现适合目的的化学探针。该平台在一组oGPCR上的应用导致发现了第一个报道的GPR39小分子激动剂,GPR39是一种与胰岛素分泌调节和胰腺β细胞保存有关的受体。化合物1以GPR39特异性的方式刺激了重组细胞和天然细胞中的细胞内钙动员,但并未增强人胰岛制剂中葡萄糖刺激的胰岛素分泌。

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