GPCR Agonists and Antagonists in the Clinic

G蛋白偶联受体 药效团 计算生物学 视紫红质样受体 受体 视紫红质 生物 药理学 生物信息学 医学 谷氨酸受体 代谢受体 生物化学 视网膜
作者
Joel D. A. Tyndall,Radhika Sandilya
出处
期刊:Medicinal Chemistry [Bentham Science Publishers]
卷期号:1 (4): 405-421 被引量:95
标识
DOI:10.2174/1573406054368675
摘要

This review describes current and new therapeutic agonists and antagonists of G-protein-coupled receptors (GPCRs) currently used in the clinic. GPCRs are classified under the GRAFS system (Glutamate, Rhodopsin, Adhesion, Frizzled/taste2 and Secretin), with therapies having been developed for about 30 GPCRs from the glutamate, rhodopsin and secretin families. Most of these therapies target the biogenic amine receptors of the rhodopsin family. Advancing technology has assisted in the identification of an increasing number of GPCRs, as well as contributing to the understanding of function and potential as pharmaceutical targets. With this has come the development of new therapies that target specific GPCRs, including peptide activated GPCRs. Where possible, agonists and antagonists are described individually, focusing on new therapies and their corresponding target receptors. However, the large number of reported biogenic amine therapies precludes, discussion of individual compounds and instead, they are discussed in relation to the receptor pharmacophore. Despite the large number of significant physiological responses known to be mediated by GPCRs, only about 4% of known GPCRs are currently targeted by therapeutics. This provides a great number of promising new targets for pharmaceutical development. Keywords: gpcr, agonist, antagonist, drugs, clinic, review, prostanoid, angiotensin, cholecystokinin, endothelin

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