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Dual modulation effects of Mas-related gene (Mrg) receptors on pain sensitivity in rats

机译:Mas相关基因(Mrg)受体对大鼠疼痛敏感性的双重调节作用

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摘要

Mas-related gene G protein-coupled (Mrg) receptors have been identified to be uniquely distributed in subpopulations of small-diameter neurons in dorsal root and trigeminal ganglia in rodents and humans. It has been demonstrated that the activation of MrgC receptors in rodents inhibits pathological pain but does not alter pain sensitivity under normal conditions. . In vitro studies have suggested that the activation of MrgX1 or MrgD receptors is associated with dual G proteins. The current study was designed to determine whether rat MrgC receptors are coupled to Gi/o and Gq proteins and what pain behavior response activation of these proteins could mediate. Intrathecal (i.t.) administration of bovine adrenal medulla 8-22 (BAM8-22), a specific MrgC receptor agonist, dose-dependently decreased tail flick latency (TFL) in rats pretreated with pertussis toxin, but not with saline. On the other hand, i.t. injected BAM8-22 increased TFL in the presence of U73122 but produced no changes in TFL following pretreatment with saline. The results in the present study provide . in vivo evidence that both Gi/o and Gq proteins are involved in MrgC receptor signaling.
机译:与Mas相关的基因G蛋白偶联(Mrg)受体已被确定独特地分布在啮齿动物和人的背根和三叉神经节的小直径神经元亚群中。已经证明,啮齿动物中MrgC受体的活化抑制病理性疼痛,但在正常条件下不会改变疼痛敏感性。 。体外研究表明,MrgX1或MrgD受体的激活与双重G蛋白有关。当前的研究旨在确定大鼠MrgC受体是否与Gi / o和Gq蛋白偶联,以及这些蛋白的疼痛行为反应激活可以介导什么。鞘内(i.t.)牛百日咳肾上腺髓质8-22(BAM8-22),一种特定的MrgC受体激动剂,剂量依赖性地降低了经百日咳毒素而非盐水预处理的大鼠的甩尾潜伏期(TFL)。另一方面,i.t。在存在U73122的情况下,注射的BAM8-22可使TFL升高,但用盐水预处理后TFL却没有变化。本研究结果提供。体内证据表明Gi / o和Gq蛋白均参与MrgC受体信号传导。

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