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P物质(1-7),一种P物质代谢产物,可抑制吗啡依赖小鼠的戒断跳跃反应。

Substance P-(1-7), a substance P metabolite, inhibits withdrawal jumping in morphine-dependent mice.

作者信息

Kreeger J S, Larson A A

机构信息

Department of Veterinary PathoBiology, University of Minnesota, St. Paul 55108.

出版信息

Eur J Pharmacol. 1993 Jul 6;238(1):111-5. doi: 10.1016/0014-2999(93)90513-h.

Abstract

Substance P has been previously shown to inhibit the intensity of the morphine abstinence syndrome in mice. In view of the rapid degradation of substance P after its release from nerve terminals, we hypothesized that this inhibition is mediated by the N-terminus of substance P and its metabolites rather than via the C-terminus interacting with neurokinin receptors. Intrathecal injection of substance P-(1-7) (1 nmol) 30 min prior to naloxone challenge, in mice that had received 25 micrograms of morphine sulfate intrathecally once daily for three days, caused a dose-related attenuation of withdrawal jumping. In contrast, administration of the substance P-(1-7) antagonist, [D-Pro2,D-Phe7]substance P-(1-7), 15 min prior to naloxone increased withdrawal jumping behaviors. Equimolar doses of morphine and naloxone at 30 min had no effect. From these data, it appears that substance P N-terminal metabolites modulate withdrawal behaviors in morphine-dependent mice.

摘要

先前已证明P物质可抑制小鼠吗啡戒断综合征的强度。鉴于P物质从神经末梢释放后迅速降解,我们推测这种抑制作用是由P物质的N端及其代谢产物介导的,而不是通过C端与神经激肽受体相互作用介导的。在每天鞘内注射25微克硫酸吗啡,连续注射三天的小鼠中,在纳洛酮激发前30分钟鞘内注射P物质(1-7)(1纳摩尔),可导致戒断跳跃呈剂量相关的减弱。相反,在纳洛酮前15分钟给予P物质(1-7)拮抗剂[D-Pro2,D-Phe7]P物质(1-7),可增加戒断跳跃行为。在30分钟时给予等摩尔剂量的吗啡和纳洛酮则没有效果。从这些数据来看,P物质N端代谢产物似乎可调节吗啡依赖小鼠的戒断行为。

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