McGaraughty Steve, Honore Prisca, Wismer Carol T, Mikusa Joseph, Zhu Chang Z, McDonald Heath A, Bianchi Bruce, Faltynek Connie R, Jarvis Michael F
Neuroscience Research, Global Pharmaceutical Research and Development, Abbott Laboratories, R4PM, AP9-1, 100 Abbott Park Road, Abbott Park, IL 60064, U.S.A.
Br J Pharmacol. 2005 Sep;146(2):180-8. doi: 10.1038/sj.bjp.0706346.
P2X3/P2X2/3 receptors have emerged as important components of nociception. However, there is limited information regarding the neurochemical systems that are affected by antagonism of the P2X3/P2X2/3 receptor and that ultimately contribute to the ensuing antinociception. In order to determine if the endogenous opioid system is involved in this antinociception, naloxone was administered just prior to the injection of a selective P2X3/P2X2/3 receptor antagonist, A-317491, in rat models of neuropathic, chemogenic, and inflammatory pain. Naloxone (1-10 mg kg(-1), i.p.), dose-dependently reduced the antinociceptive effects of A-317491 (1-300 micromol kg(-1), s.c.) in the CFA model of thermal hyperalgesia and the formalin model of chemogenic pain (2nd phase), but not in the L5-L6 spinal nerve ligation model of neuropathic allodynia. In comparison experiments, the same doses of naloxone blocked or attenuated the actions of morphine (2 or 8 mg kg(-1), s.c.) in each of these behavioral models. Injection of a peripheral opioid antagonist, naloxone methiodide (10 mg kg(-1), i.p.), did not affect A-317491-induced antinociception in the CFA and formalin assays, suggesting that the opioid component of this antinociception occurred within the CNS. Furthermore, this utilization of the central opioid system could be initiated by antagonism of spinal P2X3/P2X2/3 receptors since the antinociceptive actions of intrathecally delivered A-317491 (30 nmol) in the formalin model were reduced by both intrathecally (10-50 nmol) and systemically (10 mg kg(-1), i.p.) administered naloxone. This utilization of the opioid system was not specific to A-317491 since suramin-, a nonselective P2X receptor antagonist, induced antinociception was also attenuated by naloxone. In in vitro studies, A-317491 (3-100 microM) did not produce any agonist response at delta opioid receptors expressed in NG108-15 cells. A-317491 had been previously shown to be inactive at the kappa and mu opioid receptors. Furthermore, naloxone, at concentrations up to 1 mM, did not compete for [3H] A-317491 binding in 1321N1 cells expressing human P2X3 receptors. Taken together, these results indicate that antagonism of spinal P2X3/P2X2/3 receptors results in an indirect activation of the opioid system to alleviate inflammatory hyperalgesia and chemogenic nociception.
P2X3/P2X2/3受体已成为伤害感受的重要组成部分。然而,关于受P2X3/P2X2/3受体拮抗作用影响并最终导致随后抗伤害感受的神经化学系统的信息有限。为了确定内源性阿片系统是否参与这种抗伤害感受,在神经性、化学性和炎性疼痛的大鼠模型中,在注射选择性P2X3/P2X2/3受体拮抗剂A-317491之前立即给予纳洛酮。在热痛觉过敏的CFA模型和化学性疼痛(第二阶段)的福尔马林模型中,纳洛酮(1-10mg kg(-1),腹腔注射)剂量依赖性地降低了A-317491(1-300μmol kg(-1),皮下注射)的抗伤害感受作用,但在神经性异常性疼痛的L5-L6脊神经结扎模型中未降低。在比较实验中,相同剂量的纳洛酮在这些行为模型中的每一个中均阻断或减弱了吗啡(2或8mg kg(-1),皮下注射)的作用。注射外周阿片拮抗剂甲基碘化纳洛酮(10mg kg(-1),腹腔注射)在CFA和福尔马林试验中不影响A-317491诱导的抗伤害感受,表明这种抗伤害感受的阿片成分发生在中枢神经系统内。此外,由于鞘内注射的A-317491(30nmol)在福尔马林模型中的抗伤害感受作用被鞘内(10-50nmol)和全身(10mg kg(-1),腹腔注射)给予的纳洛酮降低,因此这种中枢阿片系统的利用可能由脊髓P2X3/P2X2/3受体的拮抗作用引发。阿片系统的这种利用并非A-317491所特有,因为非选择性P2X受体拮抗剂苏拉明诱导的抗伤害感受也被纳洛酮减弱。在体外研究中,A-317491(3-100μM)在NG108-15细胞中表达的δ阿片受体上未产生任何激动剂反应。先前已证明A-317491在κ和μ阿片受体上无活性。此外,浓度高达1mM的纳洛酮在表达人P2X3受体的1321N1细胞中不竞争[3H]A-317491结合。综上所述,这些结果表明脊髓P2X3/P2X2/3受体的拮抗作用导致阿片系统的间接激活,以减轻炎性痛觉过敏和化学性伤害感受。
