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本文引用的文献

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The cardiac sphincter in the cat.猫的贲门括约肌。
Gut. 1961 Sep;2(3):252-62. doi: 10.1136/gut.2.3.252.
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The innervation of the cardia and lower oesophagus in man.人类贲门和食管下段的神经支配。
Br J Surg. 1960 Mar;47:466-72. doi: 10.1002/bjs.18004720503.
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Pharmacologic evidence for a cardiac sphincter mechanism in the cat.
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The liberation of adenosine triphosphate on antidromic stimulation of sensory nerves.感觉神经逆向刺激时三磷酸腺苷的释放。
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Esophageal motility.食管动力
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Cardiac sympathetic adrenergic pathways in which synaptic transmission is blocked by atropine sulfate.心脏交感肾上腺素能通路,其中突触传递被硫酸阿托品阻断。
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7
Transmission of preganglionic impulses through the muscarinic receptors of the superior cervical ganglion of the cat.节前冲动通过猫颈上神经节的毒蕈碱受体的传递。
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8
Achalasia of the cardia: pharmacology and histopathology of isolated cardiac sphincteric muscle from patients with and without achalasia.贲门失弛缓症:有和无贲门失弛缓症患者的孤立贲门括约肌的药理学与组织病理学
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Esophageal responses to distension and electrical stimulation.食管对扩张和电刺激的反应。
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Effects of some autonomic drugs on circular esophageal smooth muscle.某些自主神经药物对食管环形平滑肌的作用。
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迷走神经对食管下括约肌的抑制性神经支配的性质。

Nature of the vagal inhibitory innervation to the lower esophageal sphincter.

作者信息

Goyal R K, Rattan S

出版信息

J Clin Invest. 1975 May;55(5):1119-26. doi: 10.1172/JCI108013.

DOI:10.1172/JCI108013
PMID:164484
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC301859/
Abstract

The purpose of the present study was to investigate the nature of the vagal inhibitory innervation to the lower esophageal sphincter in the anesthetized opossum. Sphincter relaxation with electrical stimulation of the vagus was not antagonized by atropine, propranolol, phentolamine, or by catechloamine depletion with reserpine. A combination of atropine and propranolol was also ineffective, suggesting that the vagal inhibitory influences may be mediated by the noncholinergic, nonadrenergic neurons. To determine whether a synaptic link with nicotinic transmission was present, we investigated the effect of hexamethonium on vagal-stimulated lower esophageal sphincter relaxation. Hexamethonium in doses that completely antagonized the sphincter relaxation in response to a ganglionic stimulant, 1,1-dimethyl-4-phenylpiperazinium iodide (DMPP), did not block the sphincter relaxation in response to vagal stimulation at 10 pulses per second, and optimal frequency of stimulation. A combination of hexamethonium and catecholamine depletion was also ineffective, but hexamethonium plus atropine markedly antagonized sphincter relaxation (P less than 0.001). Moreover, 4-(m-chlorophenyl carbamoyloxy)-2-butyltrimethylammonium chloride (McN-A-343), a muscarinic ganglionic stimulant, also caused relaxation of the lower esophageal sphincter. We suggest from these results that: (a) pthe vagal inhibitory pathway to the sphincter consists of preganglionic fibers which synapse with postganglionic neurons: (b) the synaptic transmission is predominantly cholinergic and utilizes nicotinic as well as muscarinic receptors on the postganglionic neuron, and; (c) postganglionic neurons exert their influence on the sphincter by an unidentified inhibitory transmitter that is neither adrenergic nor cholinergic.

摘要

本研究的目的是探讨麻醉负鼠下食管括约肌迷走神经抑制性神经支配的性质。迷走神经电刺激引起的括约肌松弛不受阿托品、普萘洛尔、酚妥拉明的拮抗,也不受利血平导致的儿茶酚胺耗竭的影响。阿托品和普萘洛尔联合使用也无效,提示迷走神经的抑制作用可能由非胆碱能、非肾上腺素能神经元介导。为了确定是否存在与烟碱传递的突触联系,我们研究了六甲铵对迷走神经刺激引起的下食管括约肌松弛的影响作用。六甲铵能完全拮抗神经节兴奋剂碘化1,1 - 二甲基 - 4 - 苯基哌嗪(DMPP)引起的括约肌松弛,但在每秒10次脉冲和最佳刺激频率下,六甲铵并不阻断迷走神经刺激引起的括约肌松弛。六甲铵与儿茶酚胺耗竭联合使用也无效,但六甲铵加阿托品能显著拮抗括约肌松弛(P小于0.001)。此外,毒蕈碱性神经节兴奋剂氯化4 - (间氯苯基氨甲酰氧基)- 2 - 丁基三甲基铵(McN - A - 343)也能引起下食管括约肌松弛。从这些结果我们推测:(a)支配括约肌的迷走神经抑制通路由与节后神经元形成突触的节前纤维组成;(b)突触传递主要是胆碱能的,且在节后神经元上利用烟碱和毒蕈碱受体;(c)节后神经元通过一种既非肾上腺素能也非胆碱能的未知抑制性递质对括约肌发挥作用。