Endocytic proteins mediating GPR15 receptor internalization provide insight into the underlying mechanisms

Author:

Deng Yufang1,Moo Ee Von1,Inoue Asuka2,Bräuner‐Osborne Hans1ORCID

Affiliation:

1. Department of Drug Design and Pharmacology, Faculty of Health and Medical Sciences University of Copenhagen Denmark

2. Molecular and Cellular Biochemistry, Graduate School of Pharmaceutical Sciences Tohoku University Sendai Japan

Abstract

GPR15 is a G protein‐coupled receptor involved in immune disorders such as human immunodeficiency virus‐induced enteropathy, multiple sclerosis, and colitis. Yet, the important endocytosis mechanism of GPR15 remained unclear. This study determined the participation of endocytic machinery proteins, including Gα proteins, G protein‐coupled receptor kinases (GRKs), protein kinase C, arrestins, clathrin, caveolin, and dynamin in GPR15 internalization. The results demonstrate that GPR15 internalization is moderately dependent on GRKs and clathrin, and highly dependent on caveolin and dynamin. Moreover, a bystander arrestin recruitment assay showed that GPR15 recruits arrestin‐3 to the cell membrane upon agonist stimulation, although GPR15 internalizes in an arrestin‐independent manner. Overall, our study provides novel insights into β‐arrestin recruitment and receptor internalization mechanisms for the recently deorphanized GPR15.

Funder

Carlsbergfondet

China Scholarship Council

Novo Nordisk Fonden

Publisher

Wiley

Subject

Cell Biology,Genetics,Molecular Biology,Biochemistry,Structural Biology,Biophysics

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