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P2X2 knockout mice and P2X2/P2X3 double knockout mice reveal a role for the P2X2 receptor subunit in mediating multiple sensory effects of ATP

机译:P2X2基因敲除小鼠和P2X2 / P2X3双基因敲除小鼠揭示了P2X2受体亚基在介导ATP的多种感觉作用中的作用

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摘要

Extracellular ATP plays a role in nociceptive signalling and sensory regulation of visceral function through ionotropic receptors variably composed of P2X2 and P2X3 subunits. P2X2 and P2X3 subunits can form homomultimeric P2X2, homomultimeric P2X3, or heteromultimeric P2X2/3 receptors. However, the relative contribution of these receptor subtypes to afferent functions of ATP in vivo is poorly understood. Here we describe null mutant mice lacking the P2X2 receptor subunit (P2X2−/−) and double mutant mice lacking both P2X2 and P2X3 subunits (P2X2/P2X3Dbl−/−), and compare these with previously characterized P2X3−/− mice. In patch-clamp studies, nodose, coeliac and superior cervical ganglia (SCG) neurones from wild-type mice responded to ATP with sustained inward currents, while dorsal root ganglia (DRG) neurones gave predominantly transient currents. Sensory neurones from P2X2−/− mice responded to ATP with only transient inward currents, while sympathetic neurones had barely detectable responses. Neurones from P2X2/P2X3Dbl−/− mice had minimal to no response to ATP. These data indicate that P2X receptors on sensory and sympathetic ganglion neurones involve almost exclusively P2X2 and P2X3 subunits. P2X2−/− and P2X2/P2X3Dbl−/− mice had reduced pain-related behaviours in response to intraplantar injection of formalin. Significantly, P2X3−/−, P2X2−/−, and P2X2/P2X3Dbl−/− mice had reduced urinary bladder reflexes and decreased pelvic afferent nerve activity in response to bladder distension. No deficits in a wide variety of CNS behavioural tests were observed in P2X2−/− mice. Taken together, these data extend our findings for P2X3−/− mice, and reveal an important contribution of heteromeric P2X2/3 receptors to nociceptive responses and mechanosensory transduction within the urinary bladder.
机译:细胞外ATP通过可变地由P2X2和P2X3亚基组成的离子受体在伤害性信号传导和内脏功能的感觉调节中发挥作用。 P2X2和P2X3亚基可以形成同型多聚体P2X2,同型多聚体P2X3或异型多聚体P2X2 / 3受体。但是,这些受体亚型对体内ATP传入功能的相对贡献了解甚少。在这里,我们描述了缺少P2X2受体亚基的无效突变小鼠(P2X2- /)和缺少P2X2和P2X3亚基的双重突变小鼠(P2X2 / P2X3Dbl-/-),并将它们与以前鉴定的P2X3-/-小鼠进行了比较。在膜片钳研究中,来自野生型小鼠的结节,腹腔和上颈神经节(SCG)神经元对ATP产生持续的内向电流,而背根神经节(DRG)神经元则主要产生瞬时电流。来自P2X2-/-小鼠的感觉神经元仅对瞬时内向电流对ATP做出反应,而交感神经元几乎没有可检测到的反应。来自P2X2 / P2X3Dbl-/-小鼠的神经元对ATP的反应很小甚至没有。这些数据表明,感觉和交感神经节神经元上的P2X受体几乎仅涉及P2X2和P2X3亚基。 P2X2-/-和P2X2 / P2X3Dbl-/-小鼠因足底注射福尔马林而引起的疼痛相关行为减少。值得注意的是,P2X3-/-,P2X2-/-和P2X2 / P2X3Dbl-/-小鼠因膀胱扩张而降低了膀胱反射,并降低了盆腔传入神经活动。在P2X2-/-小鼠中,未在各种CNS行为测试中发现缺陷。综上所述,这些数据扩展了我们对P2X3-/-小鼠的发现,并揭示了异聚P2X2 / 3受体对膀胱内伤害性反应和机械感觉转导的重要贡献。

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