刺激
神经科学
痛觉过敏
外围设备
小胶质细胞
止痛药
伤害
中枢神经系统
医学
炎症
生物
类阿片
药理学
伤害感受器
受体
慢性疼痛
神经炎症
免疫学
内科学
作者
Qiansen Zhang,Yimin Ren,Yiqing Mo,Peipei Guo,Ping Liao,Yuncheng Luo,Jie Mei,Zhuo Chen,Yang Zhang,Ya Li,Linghui Yang,Daqing Liao,Jie Fu,Ji Shen,Wei Huang,Xuewen Xu,Yanyan Guo,Lianghe Mei,Yunxia Zuo,Jin Liu,Huaiyu Yang,Ruotian Jiang
出处
期刊:Cell Research
[Springer Nature]
日期:2022-02-03
卷期号:32 (5): 461-476
被引量:25
标识
DOI:10.1038/s41422-022-00616-y
摘要
Both opioids and nonsteroidal anti-inflammatory drugs (NSAIDS) produce deleterious side effects and fail to provide sustained relief in patients with chronic inflammatory pain. Peripheral neuroinflammation (PN) is critical for initiation and development of inflammatory pain. A better understanding of molecular mechanisms underlying PN would facilitate the discovery of new analgesic targets and the development of new therapeutics. Emerging evidence suggests that peripheral sensory neurons are not only responders to painful stimuli, but are also actively engaged in inflammation and immunity, whereas the intrinsic regulatory mechanism is poorly understood. Here we report the expression of proton-selective ion channel Hv1 in peripheral sensory neurons in rodents and humans, which was previously shown as selectively expressed in microglia in mammalian central nervous system. Neuronal Hv1 was up-regulated by PN or depolarizing stimulation, which in turn aggravates inflammation and nociception. Inhibiting neuronal Hv1 genetically or by a newly discovered selective inhibitor YHV98-4 reduced intracellular alkalization and ROS production in inflammatory pain, mitigated the imbalance in downstream SHP-1-pAKT signaling, and also diminished pro-inflammatory chemokine release to alleviate nociception and morphine-induced hyperalgesia and tolerance. Thus, our data reveal neuronal Hv1 as a novel target in analgesia strategy and managing opioids-related side effects.
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