GPR55: Current Knowledge and Future Perspectives of a Purported "Type-3" Cannabinoid Receptor

被引:56
|
作者
Moriconi, A. [2 ]
Cerbara, I. [1 ]
Maccarrone, M. [3 ,4 ,5 ]
Topai, A. [1 ]
机构
[1] Colosseum Combinatorial Chem Ctr Technol C4T SCa, I-00173 Rome, Italy
[2] Dompe Pha Rma Spa, Res Ctr, I-67100 Laquila, Italy
[3] Univ Teramo, Dept Biomed Sci, I-64100 Teramo, Italy
[4] Santa Lucia Fdn, European Ctr Brain Res CERC, I-00143 Rome, Italy
[5] Univ Roma Tor Vergata, Dept Expt Med & Biochem Sci, I-00133 Rome, Italy
关键词
Cannabinoid receptors; functional selectivity; GPCR; GPR55; downstream signalling pathway; INCREASES INTRACELLULAR CALCIUM; CHRONIC CONSTRICTION INJURY; PROTEIN-COUPLED RECEPTORS; CB2; RECEPTOR; DIFFERENTIAL EXPRESSION; MESENTERIC VASODILATION; SELECTIVE LIGANDS; CRYSTAL-STRUCTURE; MICROGLIAL CELLS; NATURAL LIGAND;
D O I
10.2174/092986710790980069
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
In the last decade, accumulated evidence highlighted that GPR55 might be activated by several classical cannabinoid ligands, making this orphan receptor the main candidate to be considered as the "third" cannabinoid receptor. The investigation of its pharmacology has often provided divergent and more intricate results, that have complicated the understanding of the physiological role of GPR55. Nevertheless, the patent analysis regarding GPR55 outlines the fair interest of big pharmaceutical companies, especially in the first years of this decade. This investigation provides a brief overview of the current "state of the art" of our knowledge of GPR55, giving particular emphasis to its functional selectivity. This property could account for controversial roles of GPR55, whose pharmacology and downstream signaling is known to vary significantly both in ligand-and system-dependent manners. In addition, we gain insights into the challenging aspect of finding out novel GPR55 modulators, by analyzing conserved structural and functional motifs that, together with future studies, could help to elucidate its mechanism of action and to design more selective and potent small-molecules directed towards GPR55. Preliminary data highlight remarkable differences, but also intriguing commonalities, between GPR55 and other members of class A G-protein-coupled receptors. It is anticipated that, in the next future, novel lead candidates targeting GPR55 could represent new tools to better understand GPR55-mediated human diseases and, hopefully, generate an innovative class of effective next-generation therapeutics.
引用
收藏
页码:1411 / 1429
页数:19
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