Satellite glial GPR37L1 and its ligand maresin 1 regulate potassium channel signaling and pain homeostasis
Sangsu Bang, … , Luda Diatchenko, Ru-Rong Ji
Sangsu Bang, … , Luda Diatchenko, Ru-Rong Ji
Published March 26, 2024
Citation Information: J Clin Invest. 2024;134(9):e173537. https://doi.org/10.1172/JCI173537.
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Satellite glial GPR37L1 and its ligand maresin 1 regulate potassium channel signaling and pain homeostasis

Abstract

G protein–coupled receptor 37-like 1 (GPR37L1) is an orphan GPCR with largely unknown functions. Here, we report that Gpr37l1/GRP37L1 ranks among the most highly expressed GPCR transcripts in mouse and human dorsal root ganglia (DRGs) and is selectively expressed in satellite glial cells (SGCs). Peripheral neuropathy induced by streptozotoxin (STZ) and paclitaxel (PTX) led to reduced GPR37L1 expression on the plasma membrane in mouse and human DRGs. Transgenic mice with Gpr37l1 deficiency exhibited impaired resolution of neuropathic pain symptoms following PTX- and STZ-induced pain, whereas overexpression of Gpr37l1 in mouse DRGs reversed pain. GPR37L1 is coexpressed with potassium channels, including KCNJ10 (Kir4.1) in mouse SGCs and both KCNJ3 (Kir3.1) and KCNJ10 in human SGCs. GPR37L1 regulates the surface expression and function of the potassium channels. Notably, the proresolving lipid mediator maresin 1 (MaR1) serves as a ligand of GPR37L1 and enhances KCNJ10- or KCNJ3-mediated potassium influx in SGCs through GPR37L1. Chemotherapy suppressed KCNJ10 expression and function in SGCs, which MaR1 rescued through GPR37L1. Finally, genetic analysis revealed that the GPR37L1-E296K variant increased chronic pain risk by destabilizing the protein and impairing the protein’s function. Thus, GPR37L1 in SGCs offers a therapeutic target for the protection of neuropathy and chronic pain.

Authors

Sangsu Bang, Changyu Jiang, Jing Xu, Sharat Chandra, Aidan McGinnis, Xin Luo, Qianru He, Yize Li, Zilong Wang, Xiang Ao, Marc Parisien, Lorenna Oliveira Fernandes de Araujo, Sahel Jahangiri Esfahani, Qin Zhang, Raquel Tonello, Temugin Berta, Luda Diatchenko, Ru-Rong Ji

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Figure 8

GPR37L1 rare variant effects in chronic pain.

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GPR37L1 rare variant effects in chronic pain. (A) The 8 chronic pain si...
(A) The 8 chronic pain sites found in the UK Biobank project. Abdo, abdomen. (B) Volcano plot showing rare variants’ significance as a function of effect size. Each dot represents a variant. The vertical bar indicates the null effect, while the dotted horizontal bar indicates the threshold for an FDR of 20%. Two significant variants were identified: rs148475636 (blue) and rs767987863 (pink). (C) Forest plot for variant rs148475636. (D) Forest plot for variant rs767987863. The forest plots show variants’ effects at the 8 chronic pain sites. Segments track a 95% CI for point estimates of odds ratios. Estimates are not provided for allele counts of less than 5. Meta estimate from a meta-analysis of all available pain sites. Segments are colored (blue/pink) when P < 0.05.