Evidence for biased agonists and antagonists at the endothelin receptors

被引:15
|
作者
Maguire, Janet J. [1 ]
机构
[1] Addenbrookes Hosp, Expt Med & Immunotherapeut, Level 6 ACCI,Box 110, Cambridge CB2 0QQ, England
基金
英国惠康基金;
关键词
G protein coupled receptors; Endothelin; ETA; ETB; Biased agonism; Biased antagonism; beta-Arrestin; Bosentan; Pathway selectivity; IRL1620; MU-OPIOID RECEPTOR; G-PROTEIN; ETA; PEPDUCINS; RESPONSES; PEPTIDES; IRL-1620; BOSENTAN; AFFINITY; FAILURE;
D O I
10.1016/j.lfs.2016.02.069
中图分类号
R-3 [医学研究方法]; R3 [基础医学];
学科分类号
1001 ;
摘要
Biased ligands represent a new strategy for the development of more effective and better tolerated drugs. To date there has been a paucity of research exploring the potential of ligands that exhibit either G protein or beta-arrestin pathway selectivity at the endothelin receptors. Re-analysis of data may allow researchers to determine whether there is existing evidence that the endogenous ET peptides or currently available agonists and antagonists exhibit pathway bias in a particular physiological or disease setting and this is explored in the review. An alternative to molecules that bind at the orthosteric site of the ET receptors are cell penetrating peptides that interact with a segment of an intracellular loop of the receptor to modify signalling behaviour. One such peptide IC2B has been shown to have efficacy in a model of pulmonary arterial hypertension. Finally, understanding the molecular pathways that contribute to disease is critical to determining whether biased ligands will provide clinical benefit. The role of ETA signalling in ovarian cancer has been delineated in some detail and this has led to the suggestion that the development of ETA G protein biased agonists or beta-arrestin biased antagonists should be explored. (C) 2016 The Author. Published by Elsevier Inc.
引用
收藏
页码:30 / 33
页数:4
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