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ATP participates in three excitatory postsynaptic potentials in the submucous plexus of the guinea pig ileum

机译:ATP参与豚鼠回肠粘膜下丛的三种兴奋性突触后电位

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摘要

Synaptic transmission between neurones intrinsic to the wall of the intestine involves multiple neurotransmitters. This study aimed to identify neurotransmitters responsible for non-cholinergic excitatory synaptic transmission in the submucous plexus of the guinea pig ileum. Intracellular recordings were made from secretomotor and vasodilator neurones. A single electrical stimulus to a fibre tract evoked excitatory postsynaptic potentials (EPSPs) with three different time courses – fast, slow and an EPSP with an intermediate time course (latency 96 ms, duration 1.2 s). In all neurones, blocking nicotinic receptors reduced fast EPSPs, but they were abolished in only 57 of 78 neurones. Fast EPSPs were also reduced by P2 purinoceptor blockade (5 of 27 neurones) or 5-HT3 receptor blockade (3 of 20 neurones). The intermediate EPSP was abolished by P2 receptor blockade (13 of 13 neurones) or by the specific P2Y1 receptor antagonist MRS 2179 (5 of 5 neurones) and was always preceded by a nicotinic or mixed nicotinic/purinergic fast EPSP. Intermediate EPSPs were observed in over half of all neurones including most non-cholinergic secretomotor neurones identified by immunoreactivity for vasoactive intestinal peptide. The slow EPSP evoked by a single pulse stimulus was also abolished by P2 receptor blockade (5 of 5 neurones) or by MRS 2179 (3 of 3 neurones). We conclude that fast EPSPs in submucous neurones are mediated by acetylcholine acting at nicotinic receptors, ATP acting at P2X receptors and 5-HT acting at 5-HT3 receptors. Both the intermediate EPSP and the single stimulus slow EPSP are mediated by ATP acting at P2Y1 receptors.
机译:肠壁固有神经元之间的突触传递涉及多种神经递质。这项研究旨在确定负责豚鼠回肠粘膜下丛非胆碱能兴奋性突触传递的神经递质。从分泌运动和血管舒张神经元进行细胞内记录。对纤维束的单次电刺激会在三个不同的时间过程中引起兴奋性突触后电位(EPSPs)–快速,慢速和中等时间过程(潜伏期96 ms,持续时间1.2 s)。在所有神经元中,阻断烟碱样受体可降低快速的EPSP,但在78个神经元中只有57个被消除。 P2嘌呤受体阻滞(27个神经元中的5个)或5-HT3受体阻滞(20个神经元中的3个)也可降低快速EPSP。中间型EPSP被P2受体阻滞(13个神经元中的13个)或特定的P2Y1受体拮抗剂MRS 2179(5个神经元中的5个)废除,并且总是先有烟碱或烟碱/嘌呤能的快速EPSP。在所有神经元的一半以上,包括通过血管活性肠肽的免疫反应性鉴定出的大多数非胆碱能分泌运动神经元中,观察到了中间的EPSP。 P2受体阻滞(5个神经元中的5个)或MRS 2179(3个神经元中的3个)也消除了单脉冲刺激引起的慢速EPSP。我们得出的结论是,粘膜下神经元中的快速EPSP是由作用于烟碱受体的乙酰胆碱,作用于P2X受体的ATP和作用于5-HT3受体的5-HT介导的。中间EPSP和单刺激慢EPSP均由作用于P2Y1受体的ATP介导。

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