Signal Transduction Neurobiology
Orphan Receptor GPR158 Is an Allosteric Modulator of RGS7 Catalytic Activity with an Essential Role in Dictating Its Expression and Localization in the Brain*

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Regulators of G protein signaling control the duration and extent of signaling via G protein-coupled receptor (GPCR) pathways by accelerating the GTP hydrolysis on G protein α subunits thereby promoting termination of GPCR signaling. A member of this family, RGS7, plays a critical role in the nervous system where it regulates multiple neurotransmitter GPCRs that mediate vision, memory, and the action of addictive drugs. Previous studies have established that in vivo RGS7 forms mutually exclusive complexes with the membrane protein RGS7-binding protein or the orphan receptor GPR158. In this study, we examine the impact of GPR158 on RGS7 in the brain. We report that knock-out of GPR158 in mice results in marked post-transcriptional destabilization of RGS7 and substantial loss of its association with membranes in several brain regions. We further identified the RGS7-binding site in the C terminus of GPR158 and found that it shares significant homology with the RGS7-binding protein. The proximal portion of the GPR158 C terminus additionally contained a conserved sequence that was capable of enhancing RGS7 GTPase-activating protein activity in solution by an allosteric mechanism acting in conjunction with the regulators of the G protein signaling-binding domain. The distal portion of the GPR158 C terminus contained several phosphodiesterase E γ-like motifs and selectively recruited G proteins in their activated state. The results of this study establish GPR158 as an essential regulator of RGS7 in the native nervous system with a critical role in controlling its expression, membrane localization, and catalytic activity.

Background: RGS7 plays an essential role in regulating neuronal G protein signaling.

Results: Elimination of GPR158 in mice reduces RGS7 expression and membrane localization. Unique domains in GPR158 control RGS7 catalytic activity.

Conclusion: The function of RGS7 in the brain is critically regulated by binding to GPR158.

Significance: This introduces a new player and its mechanism for regulating RGS activity in the nervous system.

G Protein-coupled Receptor (GPCR)
GTPase
Heterotrimeric G Protein
Neurobiology
Regulator of G Protein Signaling (RGS)
Signal Transduction

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*

This work was supported, in whole or in part, by National Institutes of Health Grants DA036082 and DA036596 (to K. A. M.). This work was also supported by Spanish Ministry of Education and Science Grant BFU-2012-38348 and Junta de Comunidades de Castilla-La Mancha Grant PPII11-0284-9301 (to R. L.).

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© 2015 ASBMB. Currently published by Elsevier Inc; originally published by American Society for Biochemistry and Molecular Biology.