What does this research mean for the field?

GRKs and arrestins play critical roles in GPCR-dependent and -independent signaling, and adopting systematic nomenclature for these protein families offers advantages over historic naming conventions. Novelty: ClaimNovelty.SYNTHESIS. Consensus alignment: ConsensusAlignment.NEUTRAL.

What question did this study set out to answer?

The aim is to discuss the historical and current nomenclature and functions of GRKs and arrestins.

April 14, 2026Open Access

GRKs and arrestins: Nomenclature and functions in GPCR‐dependent and ‐independent signalling

Key Points

The aim is to discuss the historical and current nomenclature and functions of GRKs and arrestins.
Review of literature on mammalian GRKs and arrestins
Analysis of the structural features of the protein families
Comparison between GPCR-dependent and -independent functions
Both historic and systematic names for GRKs and arrestins are still in use.
GRKs and arrestins are crucial for regulating GPCR signaling.
The review illustrates the evolution of these protein names and their functional implications.

Abstract

G protein‐coupled receptor (GPCR) kinases (GRKs) and arrestins play a critical role in the regulation of GPCR signalling. Historic names of mammalian GRKs were replaced by systematic ones in the 1990s; however, both kinds of names are currently in use for mammalian arrestins. Here, we describe the history of the discovery of the members of these two protein families, their structure and GPCR‐dependent and ‐independent functions, as well as the origins of their historic names and the advantages of systematic nomenclature.

GRKs and arrestins: Nomenclature and functions in GPCR‐dependent and ‐independent signalling

Key Points

Abstract

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