Blocking microglial pannexin-1 channels alleviates morphine withdrawal in rodents

泛连接蛋白 吗啡 医学 药理学 鸦片剂 火种 小胶质细胞 戒毒 麻醉 神经科学 刺激 内科学 药品 受体 心理学 化学 炎症 生物化学 细胞内 连接蛋白 缝隙连接
作者
Nicole E. Burma,Robert P. Bonin,Heather Leduc‐Pessah,Corey Baimel,Zoe F. Cairncross,Michael Mousseau,Jhenkruthi Vijaya Shankara,Patrick L. Stemkowski,Dinara Baimoukhametova,Jaideep S. Bains,Michael C. Antle,Gerald W. Zamponi,Catherine M. Cahill,Stephanie L. Borgland,Yves De Koninck,Tuan Trang
出处
期刊:Nature Medicine [Nature Portfolio]
卷期号:23 (3): 355-360 被引量:139
标识
DOI:10.1038/nm.4281
摘要

Opiates are essential for treating pain, but termination of opiate therapy can cause a debilitating withdrawal syndrome in chronic users. To alleviate or avoid the aversive symptoms of withdrawal, many of these individuals continue to use opiates. Withdrawal is therefore a key determinant of opiate use in dependent individuals, yet its underlying mechanisms are poorly understood and effective therapies are lacking. Here, we identify the pannexin-1 (Panx1) channel as a therapeutic target in opiate withdrawal. We show that withdrawal from morphine induces long-term synaptic facilitation in lamina I and II neurons within the rodent spinal dorsal horn, a principal site of action for opiate analgesia. Genetic ablation of Panx1 in microglia abolished the spinal synaptic facilitation and ameliorated the sequelae of morphine withdrawal. Panx1 is unique in its permeability to molecules up to 1 kDa in size and its release of ATP. We show that Panx1 activation drives ATP release from microglia during morphine withdrawal and that degrading endogenous spinal ATP by administering apyrase produces a reduction in withdrawal behaviors. Conversely, we found that pharmacological inhibition of ATP breakdown exacerbates withdrawal. Treatment with a Panx1-blocking peptide (10panx) or the clinically used broad-spectrum Panx1 blockers, mefloquine or probenecid, suppressed ATP release and reduced withdrawal severity. Our results demonstrate that Panx1-mediated ATP release from microglia is required for morphine withdrawal in rodents and that blocking Panx1 alleviates the severity of withdrawal without affecting opiate analgesia.
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