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TRPA1 激动剂优先激活豚鼠食管迷走神经结伤害感受器亚型。

Preferential activation of the vagal nodose nociceptive subtype by TRPA1 agonists in the guinea pig esophagus.

机构信息

Pathophysiology, Jessenius Medical School, Comenius University, Martin, Slovakia.

出版信息

Neurogastroenterol Motil. 2011 Oct;23(10):e437-45. doi: 10.1111/j.1365-2982.2011.01768.x. Epub 2011 Aug 26.

Abstract

BACKGROUND

The TRPA1 receptor is directly activated by a wide range of chemicals including many endogenous molecules relevant for esophageal pathophysiology. We addressed the hypothesis that the TRPA1 agonists differentially activate esophageal nociceptive subtypes depending on their embryological source (neural crest or epibranchial placodes).

METHODS

Single cell RT-PCR and whole cell patch clamp recordings were performed on the vagal neurons retrogradely labeled from the guinea pig esophagus. Extracellular recordings were made in the isolated innervated esophagus preparation ex vivo.

KEY RESULTS

Single cell RT-PCR revealed that the majority of the nodose (placodes-derived) and jugular (neural crest-derived) TRPV1-positive esophageal nociceptors express TRPA1. Single fiber recording showed that the TRPA1 agonists allyl-isothiocyanate (AITC) and cinnamaldehyde were effective in inducing robust action potential discharge in the nerve terminals of nodose nociceptors, but had far less effect in jugular nociceptors (approximately fivefold less). Higher efficacy of the TRPA1 agonists to activate nodose nociceptors was confirmed in the isolated esophagus-labeled vagal neurons in the whole cell patch clamp studies. Similarly to neural crest-derived vagal jugular nociceptors, the spinal DRG nociceptors that are also neural crest-derived were only modestly activated by allyl-isothiocyanate.

CONCLUSIONS & INFERENCES: We conclude that the TRPA1 agonists are substantially more effective activators of the placodes-derived than the neural crest-derived esophageal nociceptors. Our data predict that in esophageal diseases the presence of endogenous TRPA1 activators will be preferentially signaled by the vagal nodose nociceptors.

摘要

背景

TRPA1 受体可被多种化学物质直接激活,包括许多与食管病理生理学相关的内源性分子。我们提出了这样一个假设,即根据其胚胎来源(神经嵴或脑颅嵴),TRPA1 激动剂会对食管伤害感受器亚型产生不同的激活作用。

方法

对豚鼠食管逆行标记的迷走神经元进行单细胞 RT-PCR 和全细胞膜片钳记录。在离体支配的食管标本上进行细胞外记录。

主要结果

单细胞 RT-PCR 显示,大多数结状神经节(颅嵴来源)和颈静脉(神经嵴来源)TRPV1 阳性食管伤害感受器表达 TRPA1。单纤维记录显示,TRPA1 激动剂丙烯基异硫氰酸酯(AITC)和肉桂醛可有效诱导结状伤害感受器神经末梢产生强动作电位放电,但对颈静脉伤害感受器的作用要小得多(约小五倍)。在全细胞膜片钳研究中,对分离的食管标记迷走神经元的研究进一步证实了 TRPA1 激动剂对结状伤害感受器的更高激活作用。与神经嵴衍生的迷走神经颈静脉伤害感受器相似,同样由神经嵴衍生的脊髓背根神经节伤害感受器也仅被丙烯基异硫氰酸酯中度激活。

结论

我们得出结论,TRPA1 激动剂对结状来源的食管伤害感受器的激活作用明显强于神经嵴来源的伤害感受器。我们的数据预测,在食管疾病中,内源性 TRPA1 激活剂将优先由迷走神经结状伤害感受器发出信号。

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