Abstract
Despite the fact that G protein-coupled receptors (GPCRs) are the largest signal-conveying receptor family and mediate many physiological processes, their role in tumor biology is underappreciated. Numerous lines of evidence now associate GPCRs and their downstream signaling targets in cancer growth and development. Indeed, GPCRs control many features of tumorigenesis, including immune cell-mediated functions, proliferation, invasion and survival at the secondary site. Technological advances have further substantiated GPCR modifications in human tumors. Among these are point mutations, gene overexpression, GPCR silencing by promoter methylation and the number of gene copies. At this point, it is imperative to elucidate specific signaling pathways of “cancer driver” GPCRs. Emerging data on GPCR biology point to functional selectivity and “biased agonism”; hence, there is a diminishing enthusiasm for the concept of “one drug per GPCR target” and increasing interest in the identification of several drug options. Therefore, determining the appropriate context-dependent conformation of a functional GPCR as well as the contribution of GPCR alterations to cancer development remain significant challenges for the discovery of dominant cancer genes and the development of targeted therapeutics.
Highlights
G protein-coupled receptors (GPCRs) comprise the largest family of cell surface receptors in the human genome, regulating a plethora of physiological responses and serving as frequent drug targets
Canonical GPCR agonist activation involves the recruitment of G proteins followed by the phosphorylation of the receptor by G protein-coupled receptor kinase (GRK), “allowing” the binding of β-arrestin 1 and 2 (e.g., referring to arrestin 2, the first non-visual arrestin, and 3, respectively) and subsequent internalization into endosomes
GPCRs are pleiotropic with respect to the cell signal proteins they activate within a cell, and more than one conformation of a receptor exists
Summary
Rachel Bar-Shavit 1,*, Myriam Maoz 1, Arun Kancharla 1, Jeetendra Kumar Nag 1, Daniel Agranovich 1, Sorina Grisaru-Granovsky 2 and Beatrice Uziely 1. Academic Editors: Kathleen Van Craenenbroeck and Gregor Drummen Received: 6 June 2016; Accepted: 8 August 2016; Published: 12 August 2016
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