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人类脊髓背角中KCC2表达降低与慢性疼痛及长期使用阿片类药物有关。

Decreased KCC2 expression in the human spinal dorsal horn associated with chronic pain and long-term opioid use.

作者信息

Davis Olivia C, Ferland Samuel, Lorenzo Louis-Etienne, Murray-Lawson Clare, Shiers Stephanie, Yousuf Muhammad Saad, Dedek Annemarie, Tsai Eve C, Vines Erin, Horton Peter, Cervantes Anna, Khan Tariq, Funk Geoffrey, Dussor Gregory, Godin Antoine G, Ferrini Francesco, De Koninck Yves, Hildebrand Michael E, Price Theodore J

机构信息

University of Texas at Dallas, Center for Advanced Pain Studies and Department of Neuroscience, Richardson, TX, United States.

Graduate Program in Neuroscience and Department of Psychiatry and Neuroscience, Université Laval, and CERVO Brain Research Centre, Quebec City, QC, Canada.

出版信息

Pain. 2025 Jul 11. doi: 10.1097/j.pain.0000000000003700.

Abstract

Loss of GABAergic and glycinergic inhibitory efficacy in the spinal dorsal horn is associated with neuropathic pain and opioid-induced hyperalgesia in rodent models. Downregulation of the KCC2 chloride extrusion transporter is a key mechanism underlying this decreased inhibitory efficacy, but to-date there is no evidence supporting or opposing this hypothesis in humans. Here, we demonstrate that KCC2 expression is decreased in superficial dorsal horn neurons of organ donors who died with a documented history of pain, or of long-term opioid use. We show profoundly decreased KCC2 dorsal horn membrane expression in a primary cohort associated with either chronic pain or opioid use, and in a replication cohort of mixed chronic pain and opioid use history. These results show that decreased dorsal horn inhibitory efficacy likely promotes chronic pain in humans and support the development of therapeutics augmenting KCC2 function as a treatment for chronic pain and opioid use disorders.

摘要

在啮齿动物模型中,脊髓背角中γ-氨基丁酸能和甘氨酸能抑制效能的丧失与神经性疼痛和阿片类药物诱导的痛觉过敏有关。钾氯共转运体2(KCC2)氯化物外排转运体的下调是这种抑制效能降低的关键机制,但迄今为止,尚无证据支持或反对人类中的这一假说。在此,我们证明,在有疼痛记录史或长期使用阿片类药物的器官捐献者的浅表背角神经元中,KCC2表达降低。我们发现,在与慢性疼痛或阿片类药物使用相关的主要队列中,以及在慢性疼痛和阿片类药物使用史混合的重复队列中,KCC2背角膜表达显著降低。这些结果表明,背角抑制效能降低可能会促进人类慢性疼痛,并支持开发增强KCC2功能的疗法,作为治疗慢性疼痛和阿片类药物使用障碍的方法。

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