神经科学
大麻素
伤害
内大麻素系统
丘脑
化学
不确定地带
大麻素受体
受体
伤害感受器
兴奋剂
心理学
生物化学
作者
Hao Wang,Ping Dong,Chao He,Xiao-Yang Feng,Yue Huang,Wei-Wei Yang,Huajing Gao,Xiao-Fan Shen,Shan Lin,Shu-Xia Cao,Hong Lian,Jiadong Chen,Min Yan,Xiao‐Ming Li
出处
期刊:Neuron
[Cell Press]
日期:2020-06-04
卷期号:107 (3): 538-551.e7
被引量:54
标识
DOI:10.1016/j.neuron.2020.04.027
摘要
Pain is a source of substantial discomfort. Abnormal activity in both the zona incerta (ZI) and posterior complex of the thalamus (Po) are implicated in neuropathic pain, but their exact roles remain unclear. In particular, the precise cell types and molecular mechanisms of the ZI-Po circuit that regulate nociception are largely uncharacterized. Here, we found that parvalbumin (PV)-positive neuronal projections from the ventral ZI (ZIv) to the Po (ZIv-Po) are critical for promoting nocifensive behaviors, whereas selectively inhibiting ZIv-Po activity reduces nocifensive withdrawal responses. Furthermore, cannabinoid type 1 receptors (CB1Rs) are expressed specifically at ZIv-Po axon terminals in this circuit, and cannabinoids attenuate nocifensive responses through presynaptic inhibition. Selective inhibition of the ZIv-Po circuit or administration of cannabinoids into the Po are sufficient to ameliorate pathological pain. These findings identify the critical role of the ZIv-Po circuit and its modulation by endocannabinoids in controlling nocifensive behaviors.
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