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吞咽的神经药理学关联:来自虚拟吞咽的启示。

Neuropharmacologic correlates of deglutition: lessons from fictive swallowing.

作者信息

Bieger D

机构信息

Faculty of Medicine, Memorial University of Newfoundland, St. John's, Canada.

出版信息

Dysphagia. 1991;6(3):147-64. doi: 10.1007/BF02493518.

DOI:10.1007/BF02493518
PMID:1680608
Abstract

Pharmacologic investigations into the transmission processes underlying fictive swallowing in the rat have disclosed the potential diversity of chemical signals used in central deglutitive pathways. Monoaminergic mechanisms appear to serve as links between subcortical structures and the medullary pattern generator of swallowing (PGS), and may play a critical role in maintaining internal facilitatory drive, required by the PGS for optimal responsivity to peripheral sensory input. Cholinergic bulbar interneurons form an integral component of the PGS subnetwork controlling esophageal peristalsis. Local GABA neurons exert a tonic inhibition of the buccopharyngeal stage, may regulate buccopharyngeal-esophageal coupling, and may contribute to peristaltic rhythmic generation at both the premotoneuronal and motoneuronal level. Receptor subtypes for excitatory amino acids (glutamate, aspartate) are differentially associated with deglutitive premotoneurons for both the buccopharyngeal and esophageal stage, as well as with ambiguus motoneurons. Preliminary evidence suggests the existence of excitatory peptidergic mechanisms involving thyrotropin-releasing hormone, vasopressin, oxytocin, and somatostatin, a probable candidate for excitatory transmitter in the solitarioambigual internuncial projection to motoneurons innervating esophageal striated musculature. Further validation of this experimental model may ultimately help to establish a framework for the clinical recognition, management, and exploitation of drug actions on central deglutitive neuroeffectors.

摘要

对大鼠虚构吞咽潜在的传递过程进行的药理学研究揭示了中枢吞咽通路中所使用化学信号的潜在多样性。单胺能机制似乎充当皮质下结构与吞咽髓质模式发生器(PGS)之间的联系,并且可能在维持PGS对周围感觉输入产生最佳反应所需的内部促进驱动方面发挥关键作用。胆碱能延髓中间神经元构成了控制食管蠕动的PGS子网络的一个组成部分。局部GABA神经元对颊咽期施加持续性抑制,可能调节颊咽-食管耦合,并且可能在运动前神经元和运动神经元水平上对蠕动节律的产生起作用。兴奋性氨基酸(谷氨酸、天冬氨酸)的受体亚型与颊咽期和食管期的吞咽运动前神经元以及疑核运动神经元存在差异关联。初步证据表明存在涉及促甲状腺激素释放激素、血管加压素、催产素和生长抑素的兴奋性肽能机制,生长抑素可能是在支配食管横纹肌的运动神经元的孤束-疑核中间神经元投射中作为兴奋性递质的候选物质。对该实验模型的进一步验证最终可能有助于建立一个框架,用于临床上识别、管理和利用药物对中枢吞咽神经效应器的作用。

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