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The TRPA1 Channel in Inflammatory and Neuropathic Pain and Migraine

机译:TRPA1通道在炎性和神经性疼痛和偏头痛中

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摘要

The transient receptor potential ankyrin 1 (TRPA1), a member of the TRP superfamily of channels, is primarily localized to a subpopulation of primary sensory neurons of the trigeminal, vagal, and dorsal root ganglia. This subset of nociceptors produces and releases the neuropeptides substance P (SP) and calcitonin gene-related peptide (CGRP), which mediate neurogenic inflammatory responses. TRPA1 is activated by a number of exogenous compounds, including molecules of botanical origin, environmental irritants, and medicines. However, the most prominent feature of TRPA1 resides in its unique sensitivity for large series of reactive byproducts of oxidative and nitrative stress. Here, the role of TRPA1 in models of different types of pain, including inflammatory and neuropathic pain and migraine, is summarized. Specific attention is paid to TRPA1 as the main contributing mechanism to the transition of mechanical and cold hypersensitivity from an acute to a chronic condition and as the primary transducing pathway by which oxidativeitrative stress produces acute nociception, allodynia, and hyperalgesia. A series of migraine triggers or medicines have been reported to modulate TRPA1 activity and the ensuing CGRP release. Thus, TRPA1 antagonists may be beneficial in the treatment of inflammatory and neuropathic pain and migraine.
机译:瞬时受体电位锚蛋白1(TRPA1),通道的TRP超家族的成员,主要位于三叉神经,迷走神经和背根神经节的主要感觉神经元的亚群。伤害感受器的这一子集产生并释放介导神经源性炎症反应的神经肽物质P(SP)和降钙素基因相关肽(CGRP)。 TRPA1被许多外源性化合物激活,包括植物来源的分子,环境刺激物和药物。但是,TRPA1的最突出特征在于其对氧化和硝化应激的大量反应副产物的独特敏感性。在此,总结了TRPA1在不同类型的疼痛模型中的作用,包括炎症性和神经性疼痛以及偏头痛。特别要注意TRPA1,它是机械性和冷性超敏反应从急性状态转变为慢性状态的主要作用机制,并且是氧化/硝化应激产生急性痛觉,异常性疼痛和痛觉过敏的主要转导途径。据报道,一系列偏头痛触发剂或药物可调节TRPA1活性和随后的CGRP释放。因此,TRPA1拮抗剂可能对炎性和神经性疼痛和偏头痛的治疗有益。

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