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首页> 外文期刊>Pharmacology, Biochemistry and Behavior >P2Y receptors in neuropathic pain
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P2Y receptors in neuropathic pain

机译:神经性疼痛中的P2Y受体

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This review summarizes and evaluates the relationship between neuropathic pain and P2Y receptors from inception to 2019. Purinergic receptors have been well studied in recent years using various molecular biological methods. The main research objective of this review is to determine the association of P2Y1, P2Y2, P2Y6, P2Y12 and P2Y13 receptors with neuropathic pain. This review includes the most comprehensive subtypes of P2Y that related to neuropathic pain and the current therapeutic method of neuropathic pain. G protein-coupled P2Y receptors are located on neurons, astrocytes, oligodendrocytes and microglial cells and regulate neuro-transmission. Nerve injury is the prime reason for abnormal regulation of P2Y receptor mRNA expression, subsequently, inducing neuropathic pain. Neuropathic pain is a type of chronic pain that is divided into peripheral, central and mixed. Numerous studies demonstrated a positive correlation between the expression level of P2Y receptors and neuropathic pain generation. Also, several reports showed that P2Y short hairpin RNA (shRNA) and P2Y antagonist can be used as an analgesic to relieve neuropathic pain via decreasing P2Y receptor expression level and neural cell activation. However, the transformation process from basic experiments to clinical applications is a long process. Current deficiencies and future research directions are discussed at the end of this review.
机译:本综述总结和评估了从初始到2019年的神经性疼痛和P2Y受体之间的关系。近年来使用各种分子生物方法研究了嘌呤能受体。本综述的主要研究目的是确定P2Y1,P2Y2,P2Y6,P2Y12和P2Y13受体具有神经性疼痛的关联。该综述包括与神经病疼痛和神经性疼痛的当前治疗方法相关的最全面的P2Y亚型。 G蛋白偶联的P2Y受体位于神经元,星形胶质细胞,少峰细胞和小胶质细胞上并调节神经传递。神经损伤是P2Y受体mRNA表达异常调节的主要原因,随后诱导神经性疼痛。神经性疼痛是一种慢性疼痛,分为外周,中央和混合。许多研究证明了P2Y受体的表达水平与神经性疼痛产生之间的正相关性。此外,若干报告显示,P2Y短发夹RNA(ShRNA)和P2Y拮抗剂可以用作镇痛剂通过降低P2Y受体表达水平和神经细胞活化来缓解神经性疼痛。然而,从基本实验到临床应用的转化过程是一个很长的过程。本次审查结束时讨论了当前的缺陷和未来的研究方向。

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