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GPR39 regulated spinal glycinergic inhibition and mechanical inflammatory pain

Hu-Hu Bai, Kangli Wang, Xiang-Ru Zeng, Jing Li, Yuan Li, Jia-Yu Xu, Yue Zhang, Haifeng Jiang, Xian Yang, Zhan‐Wei Suo, Xiao‐Dong Hu

2024Science Advances14 citationsDOIOpen Access PDF

Abstract

G protein–coupled receptor 39 (GPR39) senses the change of extracellular divalent zinc ion and signals through multiple G proteins to a broad spectrum of downstream effectors. Here, we found that GPR39 was prevalent at inhibitory synapses of spinal cord somatostatin-positive (SOM + ) interneurons, a mechanosensitive subpopulation that is critical for the conveyance of mechanical pain. GPR39 complexed specifically with inhibitory glycine receptors (GlyRs) and helped maintain glycinergic transmission in a manner independent of G protein signalings. Targeted knockdown of GPR39 in SOM + interneurons reduced the glycinergic inhibition and facilitated the excitatory output from SOM + interneurons to spinoparabrachial neurons that engaged superspinal neural circuits encoding both the sensory discriminative and affective motivational domains of pain experience. Our data showed that pharmacological activation of GPR39 or augmenting GPR39 interaction with GlyRs at the spinal level effectively alleviated the sensory and affective pain induced by complete Freund’s adjuvant and implicated GPR39 as a promising therapeutic target for the treatment of inflammatory mechanical pain.

Topics & Concepts

Glycine receptorInhibitory postsynaptic potentialNeuroscienceExcitatory postsynaptic potentialSensory systemChemistryMedicineBiologyGlycineBiochemistryAmino acidPain Mechanisms and TreatmentsIon channel regulation and functionReceptor Mechanisms and Signaling
GPR39 regulated spinal glycinergic inhibition and mechanical inflammatory pain | Litcius