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与呕吐相关的中枢神经回路。

Central neurocircuitry associated with emesis.

作者信息

Hornby P J

机构信息

Department of Pharmacology, Louisiana State University Health Sciences Center, 1901 Perdido Street, New Orleans, LA 70112, USA.

出版信息

Am J Med. 2001 Dec 3;111 Suppl 8A:106S-112S. doi: 10.1016/s0002-9343(01)00849-x.

Abstract

Ingestion of toxin, traumatic events, adverse drug reactions, and motion can all result in nausea and emesis. In addition, cyclic vomiting syndrome is quite prevalent in the pediatric population. Coordination of the various autonomic changes associated with emesis occurs at the level of the medulla oblongata of the hindbrain. Chemosensitive receptors detect emetic agents in the blood and relay this information by means of neurons in the area postrema to the adjacent nucleus tractus solitarius (NTS). Abdominal vagal afferents that detect intestinal luminal contents and gastric tone also terminate in the NTS (gelatinosus, commissural, and medial subnuclei). The NTS is viscerotopically organized into subnuclei that subserve diverse functions related to swallowing (subnucleus centralis), gastric sensation (subnucleus gelatinosus), laryngeal and pharyngeal sensation (intermediate and interstitial NTS), baroreceptor function (medial NTS), and respiration (ventrolateral NTS). Neurons from the NTS project to a central pattern generator (CPG), which coordinates the sequence of behaviors during emesis, as well as directly to diverse populations of neurons in the ventral medulla and hypothalamus. Thus, it is critical to realize that there is not an isolated "vomiting center," but rather groups of loosely organized neurons throughout the medulla that may be activated in sequence by a CPG. The newer antiemetic agents appear to block receptors in the peripheral endings of vagal afferents to reduce "perception" of emetic stimuli and/or act in the dorsal vagal complex. A primary site of action of 5-HT(3)-receptor antagonists is by means of the vagal afferents. Neurokinin-1 receptor (NK(1)R) antagonists are antiemetics, because they act at a site in the dorsal vagal complex. Part of their effectiveness may be the result of inhibition of the NK(1)R on vagal motor neurons to prevent fundic relaxation, which is a prodromal event essential for emesis. Delta(9)-tetrahydrocannabinol (Delta(9)-THC), the major psychoactive component of marijuana, can be therapeutically useful as an antiemetic. The site of action of Delta(9)-THC is on cannabinoid CB1 receptors in the dorsal vagal complex. However, it decreases fundic tone and antral motility. It is not easy to predict the potential antiemetic effects of drugs that alter motility. Although antiemetic drugs are available for management of acute chemotherapeutic-induced emesis, few treatments are effective for delayed emesis or cyclic vomiting syndrome.

摘要

摄入毒素、经历创伤事件、药物不良反应和运动都可能导致恶心和呕吐。此外,周期性呕吐综合征在儿科人群中相当普遍。与呕吐相关的各种自主神经变化的协调发生在后脑延髓水平。化学感受器检测血液中的催吐剂,并通过最后区的神经元将信息传递给相邻的孤束核(NTS)。检测肠腔内容物和胃张力的腹部迷走神经传入纤维也终止于NTS(胶状、连合和内侧亚核)。NTS按内脏部位组织成亚核,这些亚核负责与吞咽(中央亚核)、胃感觉(胶状亚核)、喉和咽感觉(中间和间质NTS)、压力感受器功能(内侧NTS)和呼吸(腹外侧NTS)相关的各种功能。来自NTS的神经元投射到一个中央模式发生器(CPG),该发生器协调呕吐期间的行为序列,并直接投射到延髓腹侧和下丘脑的不同神经元群。因此,必须认识到不存在一个孤立的“呕吐中枢”,而是延髓中一组组织松散的神经元,它们可能由CPG依次激活。较新的止吐药似乎能阻断迷走神经传入纤维外周末梢的受体,以减少对催吐刺激的“感知”和/或作用于迷走背核复合体。5-羟色胺3(5-HT(3))受体拮抗剂的主要作用部位是通过迷走神经传入纤维。神经激肽-1受体(NK(1)R)拮抗剂是止吐药,因为它们作用于迷走背核复合体中的一个部位。它们的部分有效性可能是由于抑制了迷走运动神经元上的NK(1)R,以防止胃底松弛,而胃底松弛是呕吐必不可少的前驱事件。大麻的主要精神活性成分δ9-四氢大麻酚(δ9-THC)作为止吐药可能具有治疗作用。δ9-THC的作用部位是迷走背核复合体中的大麻素CB1受体。然而,它会降低胃底张力和胃窦运动性。预测改变运动性的药物的潜在止吐作用并不容易。虽然有止吐药可用于治疗急性化疗引起的呕吐,但很少有治疗方法对延迟性呕吐或周期性呕吐综合征有效。

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