低亲和力代谢中间产物 G 蛋白偶联受体:对药理学家的挑战。
Low affinity GPCRs for metabolic intermediates: challenges for pharmacologists.
机构信息
Molecular Cardiology, Victor Chang Cardiac Research Institute Darlinghurst, NSW, Australia.
出版信息
Front Endocrinol (Lausanne). 2012 Jan 13;3:1. doi: 10.3389/fendo.2012.00001. eCollection 2012.
Abstract
The discovery that a number of metabolites and metabolic intermediates can act through G protein-coupled receptors has attracted great interest in the field and has led to new therapeutic targets for diseases such as hypertension, type 2 diabetes, inflammation, and metabolic syndrome. However, the low apparent affinity of these ligands for their cognate receptors poses a number of challenges for pharmacologists interested in investigating receptor structure, function or physiology. Furthermore, the endogenous ligands matched to their receptors have other, well established metabolic roles and thus selectivity is difficult to achieve. This review discusses some of the issues researchers face when working with these receptors and highlights the ways in which a number of these obstacles have been overcome.
摘要
研究发现,许多代谢物和代谢中间产物可以通过 G 蛋白偶联受体发挥作用,这引起了该领域的极大兴趣,并为高血压、2 型糖尿病、炎症和代谢综合征等疾病提供了新的治疗靶点。然而,这些配体与它们的同源受体的低表观亲和力给对研究受体结构、功能或生理学感兴趣的药理学家带来了一些挑战。此外,与这些受体相匹配的内源性配体还有其他已经确立的代谢作用,因此很难实现选择性。这篇综述讨论了研究人员在研究这些受体时面临的一些问题,并强调了克服这些障碍的一些方法。
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