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向大鼠黑质注入阿片类药物可预防最大电休克发作。

Infusion of opiates into substantia nigra protects against maximal electroshock seizures in rats.

作者信息

Garant D S, Gale K

出版信息

J Pharmacol Exp Ther. 1985 Jul;234(1):45-8.

PMID:2989511
Abstract

Microinfusion of morphine sulfate (50 nmol), [d-Ala2]-Met-enkephalin (35 nmol) or dynorphin A 1-13 (1 nmol) bilaterally into the substantia nigra significantly attenuated seizures induced by maximal electroshock in rats. This action was accompanied by stereotyped behavioral hyperactivity. These anticonvulsant and behavioral effects were antagonized by systemic naloxone administration; neither effect was observed after intranigral microinjection of dynorphin A 1-17 amide (1 nmol). These results are consistent with a mu opiate receptor-mediated inhibition of substantia nigra efferent neurons, and with the proposal that bilateral inhibition of nigral efferents attenuates seizure propagation. However, intranigral morphine failed to alter the severity of i.v. bicuculline seizures, indicating that opiate-mediated inhibition in substantia nigra is distinct from that produced by gamma-aminobutyric acid.

摘要

双侧向大鼠黑质微量注射硫酸吗啡(50纳摩尔)、[D-丙氨酸2]-甲硫氨酸脑啡肽(35纳摩尔)或强啡肽A 1-13(1纳摩尔)可显著减轻最大电休克诱导的癫痫发作。此作用伴有刻板行为亢进。全身性给予纳洛酮可拮抗这些抗惊厥和行为效应;向黑质内微量注射强啡肽A 1-17酰胺(1纳摩尔)后未观察到任何一种效应。这些结果与μ阿片受体介导的黑质传出神经元抑制作用一致,也与双侧抑制黑质传出可减轻癫痫发作传播的观点一致。然而,向黑质内注射吗啡未能改变静脉注射荷包牡丹碱诱发癫痫的严重程度,表明黑质中阿片介导的抑制作用与γ-氨基丁酸产生的抑制作用不同。

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