Biased agonists of GPR84 and insights into biological control

Author:

Luscombe Vincent B.1ORCID,Wang Pinqi2ORCID,Russell Angela J.23ORCID,Greaves David R.1ORCID

Affiliation:

1. Sir William Dunn School of Pathology University of Oxford Oxford UK

2. Department of Chemistry University of Oxford Oxford UK

3. Department of Pharmacology University of Oxford Oxford UK

Abstract

AbstractGPR84 was first identified as an open reading frame encoding an orphan Class A G protein coupled receptor in 2001. Gpr84 mRNA is expressed in a limited number of cell types with the highest levels of expression being in innate immune cells, M1 polarised macrophages and neutrophils. The first reported ligands for this receptor were medium chain fatty acids with chain lengths between 9 and 12 carbons. Subsequently, a series of synthetic agonists that signal via the GPR84 receptor were identified. Radioligand binding assays and molecular modelling with site‐directed mutagenesis suggest the presence of three ligand binding sites on the receptor, but the physiological agonist(s) of the receptor remain unidentified. Here, we review the effects of GPR84 agonists on innate immune cells following a series of chemical discoveries since 2001. The development of highly biased agonists has helped to probe receptor function in vitro, and the remaining challenge is to follow the effects of biased signalling to the physiological functions of innate immune cell types.

Funder

Clarendon Fund

Somerville College, University of Oxford

Publisher

Wiley

Subject

Pharmacology

Cited by 2 articles. 订阅此论文施引文献 订阅此论文施引文献,注册后可以免费订阅5篇论文的施引文献,订阅后可以查看论文全部施引文献

1. Editorial for GPR84 pharmacology;British Journal of Pharmacology;2024-03-08

2. Structure–Activity Relationship Studies and Optimization of 4-Hydroxypyridones as GPR84 Agonists;Journal of Medicinal Chemistry;2024-02-21

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