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The G protein-coupled receptor repertoires of human and mouse.

机译:人类和小鼠的G蛋白偶联受体库。

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摘要

Diverse members of the G protein-coupled receptor (GPCR) superfamily participate in a variety of physiological functions and are major targets of pharmaceutical drugs. Here we report that the repertoire of GPCRs for endogenous ligands consists of 367 receptors in humans and 392 in mice. Included here are 26 human and 83 mouse GPCRs not previously identified. A direct comparison of GPCRs in the two species reveals an unexpected level of orthology. The evolutionary preservation of these molecules argues against functional redundancy among highly related receptors. Phylogenetic analyses cluster 60% of GPCRs according to ligand preference, allowing prediction of ligand types for dozens of orphan receptors. Expression profiling of 100 GPCRs demonstrates that most are expressed in multiple tissues and that individual tissues express multiple GPCRs. Over 90% of GPCRs are expressed in the brain. Strikingly, however, the profiles of most GPCRs are unique, yielding thousands of tissue- and cell-specific receptorcombinations for the modulation of physiological processes.
机译:G蛋白偶联受体(GPCR)超家族的不同成员参与多种生理功能,并且是药物的主要目标。在这里,我们报告内源性配体的GPCR的库由人类中的367个受体和小鼠中的392个受体组成。这里包括以前未鉴定的26个人和83小鼠GPCR。对两个物种中GPCR的直接比较显示出意想不到的矫正水平。这些分子的进化保存反对高度相关的受体之间的功能冗余。系统发生分析可根据配体偏好对60%的GPCR进行聚类,从而可以预测数十个孤儿受体的配体类型。 100个GPCR的表达谱表明,大多数表达在多个组织中,单个组织表达多个GPCR。超过90%的GPCR在大脑中表达。然而,令人惊讶的是,大多数GPCR的图谱是独特的,可产生数千种组织和细胞特异性受体组合,用于调节生理过程。

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