ATP-releasing SWELL1 channel in spinal microglia contributes to neuropathic pain

小胶质细胞 神经病理性疼痛 脊髓 嘌呤能受体 医学 神经损伤 周围神经损伤 痛觉超敏 药理学 脊髓损伤 细胞外 神经科学 麻醉 细胞生物学 伤害 炎症 内科学 腺苷 受体 痛觉过敏 生物 坐骨神经 精神科
作者
Jiachen Chu,Junhua Yang,Yuan Zhou,Jianan Chen,Kevin Hong Chen,Chi Zhang,Yi Cheng,Nicholas Koylass,Jun O. Liu,Yun Guan,Zhaozhu Qiu
标识
DOI:10.1101/2023.01.08.523161
摘要

Following peripheral nerve injury, extracellular ATP-mediated purinergic signaling is crucial for spinal cord microglia activation and neuropathic pain. However, the mechanisms of ATP release remain poorly understood. Here, we show that volume-regulated anion channel (VRAC) is an ATP-releasing channel and is activated by inflammatory mediator sphingosine-1-phosphate (S1P) in microglia. Mice with microglia-specific deletion of Swell1 (also known as Lrrc8a), a VRAC essential subunit, had reduced peripheral nerve injury-induced increase in extracellular ATP in spinal cord. The mutant mice also exhibited decreased spinal microgliosis, dorsal horn neuronal hyperactivity, and both evoked and spontaneous neuropathic pain-like behaviors. We further performed high-throughput screens and identified an FDA-approved drug dicumarol as a novel and potent VRAC inhibitor. Intrathecal administration of dicumarol alleviated nerve injury-induced mechanical allodynia in mice. Our findings suggest that ATP-releasing VRAC in microglia is a key spinal cord determinant of neuropathic pain and a potential therapeutic target for this debilitating disease.
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