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LPA receptor signaling as a therapeutic target for radical treatment of neuropathic pain and fibromyalgia

机译:LPA受体信号作为治疗神经性疼痛和纤维肌痛的自由基治疗的治疗靶标

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摘要

Since the first discovery that the bioactive lipid, lysophosphatidic acid (LPA) and LPA_1 receptor signaling play a role in the initiation of neuropathic pain (NeuP), accumulated reports have supported the original findings and extended the study toward possible therapeutic applications. The present review describes beneficial roles of LPA receptor signaling in a variety of chronic pain, such as peripheral NeuP induced by nerve injury, chemotherapy and diabetes, central NeuP induced by cerebral ischemia with hemorrhage and spinal cord injury, and fibromyalgia-like wide spread pain induced by repeated cold, psychological and muscular acidic stress. Emerging mechanistic findings are the feed-forward amplification of LPA production through LPA_1, LPA_3 and microglia and the evidence for maintenance of chronic pain by LPA receptor signaling.
机译:由于生物活性脂质,溶血磷脂酸(LPA)和LPA_1受体信号传导在神经病疼痛(NEUP)开始中发挥作用,因此累积的报告支持了原始调查结果并将研究扩展到可能的治疗应用。 本综述描述了LPA受体信号传导在各种慢性疼痛中的有益作用,例如由脑缺血引起的神经损伤,化疗和糖尿病诱导的外周Neup,随着出血和脊髓损伤,以及纤维肌痛的纤维状宽蔓延疼痛 反复冷,心理和肌肉酸性胁迫引起。 新兴机械发现是通过LPA_1,LPA_3和小胶质细胞的LPA产生的前馈扩增以及LPA受体信号传导维持慢性疼痛的证据。

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    《Pain management》 |2020年第1期|共11页
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  • 正文语种 eng
  • 中图分类 护理学;
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