首页> 外文期刊>Histochemistry and cell biology >Altered expression of P2X3 in vagal and spinal afferents following esophagitis in rats.
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Altered expression of P2X3 in vagal and spinal afferents following esophagitis in rats.

机译:食管炎后大鼠迷走神经和脊髓传入神经中P2X3表达的改变。

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摘要

Purinergic P2X(3) receptors are predominantly expressed in small diameter primary afferent neurons and activation of these receptors by adenosine triphosphate is reported to play an important role in nociceptive signaling. The objective of this study was to investigate the expression of P2X(3) receptors in spinal and vagal sensory neurons and esophageal tissues following esophagitis in rats. Two groups of rats were used including 7 days fundus-ligated (7D-ligated) esophagitis and sham-operated controls. Esophagitis was produced by ligating the fundus and partial obstruction of pylorus that initiated reflux of gastric contents. The sham-operated rats underwent midline incision without surgical manipulation of the stomach. Expressions of P2X(3) receptors in thoracic dorsal root ganglia (DRGs), nodose ganglia (NGs), and esophageal tissues were evaluated by RT-PCR, western blot and immunohistochemistry. Esophageal neurons were identified by retrograde transport of Fast Blue from the esophagus. There were no significant differences in P2X(3) mRNA expressions in DRGs (T1-T3) and NGs between 7D-ligated and sham-operated rats. However, there was an upregulation of P2X(3) mRNA in DRGs (T6-T12) and in the esophageal muscle. At protein level, P2X(3) exhibited significant upregulation both in DRGs and in NGs of rats having chronic esophagitis. Immunohistochemical analysis exhibited a significant increase in P2X(3) and TRPV1 co-expression in DRGs and NGs in 7D-ligated rats compared to sham-operated rats. The present findings suggest that chronic esophagitis results in upregulation of P2X(3) and its co-localization with TRPV1 receptor in vagal and spinal afferents. Changes in P2X(3) expression in vagal and spinal sensory neurons may contribute to esophageal hypersensitivity following acid reflux-induced esophagitis.
机译:Purinergic P2X(3)受体主要在小直径初级传入神经元中表达,据报道这些受体被三磷酸腺苷激活在伤害性信号传导中起重要作用。这项研究的目的是调查大鼠食管炎后脊髓和迷走感觉神经元和食管组织中P2X(3)受体的表达。使用两组大鼠,包括7天眼底结扎(7D结扎)食管炎和假手术对照组。结扎胃底和幽门部分阻塞引起胃内容物反流而产生食管炎。假手术的大鼠未经胃部手术而行中线切开。通过RT-PCR,Western印迹和免疫组化评估了胸背根神经节(DRGs),结节神经节(NGs)和食道组织中P2X(3)受体的表达。食管神经元是通过食管中的坚牢蓝逆行转运而鉴定的。没有7D结扎和假手术大鼠DRGs(T1-T3)和NGs中P2X(3)mRNA表达的显着差异。但是,DRGs(T6-T12)和食管肌肉中的P2X(3)mRNA上调。在蛋白质水平上,P2X(3)在患有慢性食管炎的大鼠的DRG和NG中均表现出明显的上调。免疫组化分析显示,与假手术大鼠相比,在7D结扎大鼠中DRGs和NGs中P2X(3)和TRPV1共表达显着增加。目前的发现表明,慢性食管炎会导致P2X(3)的上调及其与迷走神经和脊髓传入神经中TRPV1受体的共定位。迷走神经和脊髓感觉神经元中P2X(3)表达的变化可能会导致胃酸反流性食管炎后食管超敏反应。

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