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1994年联合沃尔夫奖颁奖仪式。猫的外周和中枢三叉神经血管激活被5-羟色胺(5HT)-1D受体激动剂311C90阻断。

Joint 1994 Wolff Award Presentation. Peripheral and central trigeminovascular activation in cat is blocked by the serotonin (5HT)-1D receptor agonist 311C90.

作者信息

Goadsby P J, Edvinsson L

机构信息

Department of Neurology, Prince Henry Hospital, Sydney, NSW, Australia.

出版信息

Headache. 1994 Jul-Aug;34(7):394-9. doi: 10.1111/j.1526-4610.1994.hed3407394.x.

Abstract

Migraine headache involves the activation of trigeminal afferents that are predominantly found in the first or ophthalmic division of the nerve. The headache is often pounding and the connections of the trigeminal nerve, the trigeminovascular system, have therefore been implicated in the pathophysiology of migraine and studied extensively. Considerable attention has been given to the peripheral ramifications of the system as a possible locus of action for anti-migraine drugs while little attention has been focused upon possible central sites of action. It has been shown that certain peptides can act as markers for the trigeminal system, in particular calcitonin gene-related peptide (CGRP), and that CGRP is elevated in migraine. We have employed an animal model for activation of the trigeminovascular system to evaluate a new antimigraine compound, 311C90, that may have central and as well as peripheral trigeminal actions. Cats were anesthetized by halothane induction and alpha-chloralose maintenance (60 mg/kg, intraperitoneal), intubated, paralyzed and ventilated. Biparietal craniotomies were carried out to measure cerebral blood flow using laser Doppler flowmetry (CBFLDF). The external jugular vein was cannulated and blood drawn, centrifuged and frozen until processing. Stimulation of the trigeminal ganglion resulted in a mean maximum increase in CBFLDF of 39 +/- 5% at 20/s. The 5HT1 agonist 311C90 was administered intravenously in two doses (30 and 100 micrograms/kg) to cover the range of doses likely to be effective clinically. At each dose the CBFLDF effect of trigeminal ganglion stimulation was inhibited.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

偏头痛涉及三叉神经传入纤维的激活,这些纤维主要存在于该神经的第一支或眼支。头痛通常为搏动性,因此三叉神经的连接,即三叉神经血管系统,已被认为与偏头痛的病理生理学有关,并得到了广泛研究。该系统的外周分支作为抗偏头痛药物可能的作用位点受到了相当多的关注,而对可能的中枢作用位点的关注则很少。已经表明,某些肽可以作为三叉神经系统的标志物,特别是降钙素基因相关肽(CGRP),并且CGRP在偏头痛中升高。我们采用了一种激活三叉神经血管系统的动物模型来评估一种新的抗偏头痛化合物311C90,它可能具有中枢和外周三叉神经作用。猫通过氟烷诱导和α-氯醛糖维持麻醉(60mg/kg,腹腔注射),插管、麻痹并通气。进行双侧颅骨切开术以使用激光多普勒血流仪测量脑血流量(CBF LDF)。将颈外静脉插管,抽血,离心并冷冻直至处理。以20次/秒的频率刺激三叉神经节导致CBF LDF平均最大增加39±5%。静脉注射5HT1激动剂311C90,剂量为两剂(30和100μg/kg),以涵盖临床可能有效的剂量范围。在每个剂量下,三叉神经节刺激对CBF LDF的作用均被抑制。(摘要截短于250字)

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