Emerging paradigms of β-arrestin-dependent seven transmembrane receptor signaling

Abstract

β-arrestins, originally discovered to desensitize activated seven transmembrane receptors (7TMRs; also known as G protein-coupled receptors [GPCRs]), are now well established mediators of receptor endocytosis, ubiquitylation and G protein-independent signaling. Recent global analyses of β-arrestin interactions and β-arrestin-dependent phosphorylation events have uncovered several previously unanticipated roles of β-arrestins in a range of cellular signaling events. These findings strongly suggest that the functional roles of β-arrestins are much broader than currently understood. Biophysical studies aimed at understanding multiple active conformations of the 7TMRs and the β-arrestins have begun to unravel the mechanistic basis for the diverse functional capabilities of β-arrestins in cellular signaling.