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新生大鼠长期暴露于阿片类拮抗剂纳洛酮会损害成年期皮质扩散性抑制的传播。

Chronic neonatal exposure of rats to the opioid antagonist naloxone impairs propagation of cortical spreading depression in adulthood.

作者信息

Rocha-de-Melo Ana Paula, de Lima Kalina Rimena, de Albuquerque Juliana da Mota Silveira, de Oliveira Andréa Kátia Prado, Guedes Rubem Carlos Araújo

机构信息

Departamento de Nutrição, Universidade Federal de Pernambuco, BR-50670-901, Recife, PE, Brazil.

出版信息

Neurosci Lett. 2008 Aug 29;441(3):315-8. doi: 10.1016/j.neulet.2008.06.057. Epub 2008 Jun 26.

Abstract

Naloxone is an opioid receptor antagonist with effects on the EEG and behavior in animals and humans and has been used clinically in drug-abuse treatment. The goal of this work in the rat is to determine whether treatment with naloxone during the suckling period would influence the propagation of cortical spreading depression (CSD), both in weaned young and adult animals. From the 7th to the 28th postnatal day, male rat pups were treated daily with a single subcutaneous injection of either 10mg/kg/d naloxone (n=21 rats) or equivalent volume (10ml/kg) of saline (n=16). In both treatment conditions, when the pups were 30-40 days- (young groups; 9 Naloxone- and 10 saline-treated rats), or 90-120-days old (adult groups; 12 Naloxone- and 6 saline-treated rats), a 4h CSD recording session was performed with electrodes at two points at a fixed distance apart on the parietal cortical surface. CSD propagation velocity was calculated based on the time spent for a CSD-wave to pass between the electrodes. In both young- and adult groups, naloxone-treated animals displayed lower CSD velocities (P<0.05) than the corresponding saline injected animals. Our results demonstrate, for the first time, that chronic neonatal exposure of rats to the opioid antagonist naloxone results in an impairing propagation of the CSD that is long lasting, suggesting the existence of one or more opioid-mediated processes influencing CSD.

摘要

纳洛酮是一种阿片受体拮抗剂,对动物和人类的脑电图及行为均有影响,已在药物滥用治疗中得到临床应用。本研究在大鼠身上的目的是确定哺乳期用纳洛酮治疗是否会影响断奶幼鼠和成鼠的皮质扩散性抑制(CSD)的传播。从出生后第7天到第28天,雄性幼鼠每天皮下注射一次,一组注射10mg/kg/d的纳洛酮(n = 21只大鼠),另一组注射等量体积(10ml/kg)的生理盐水(n = 16只)。在两种治疗条件下,当幼鼠30 - 40日龄时(幼鼠组;9只接受纳洛酮治疗和10只接受生理盐水治疗的大鼠),或90 - 120日龄时(成年组;12只接受纳洛酮治疗和6只接受生理盐水治疗的大鼠),在顶叶皮质表面相距固定距离的两点放置电极,进行4小时的CSD记录。根据CSD波在电极之间传播所需的时间计算CSD传播速度。在幼鼠组和成年组中,接受纳洛酮治疗的动物的CSD速度均低于相应的注射生理盐水的动物(P<0.05)。我们的结果首次表明,大鼠在新生期长期接触阿片拮抗剂纳洛酮会导致CSD传播受损,且这种影响持续时间长,提示存在一个或多个阿片介导的影响CSD的过程。

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