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慢性产前和产后给予纳曲酮对小鼠吗啡诱导的运动活动的影响。

Influence of chronic prenatal and postnatal administration of naltrexone in locomotor activity induced by morphine in mice.

作者信息

Medina Jiménez M, Luján Estrada M, Rodríguez R

机构信息

Departamento de Farmacología, Facultad de Medicina, Universidad Nacional Autónoma de México, México, D.F.

出版信息

Arch Med Res. 1997 Spring;28(1):61-5.

PMID:9078589
Abstract

The influence of chronic pre- and postnatal naltrexone exposure on the sensitivity of offspring to the locomotor effects of morphine was investigated in C-57 Black mice. Pregnant mice were injected subcutaneously (sc) with either saline (0.1 ml/10 g) or naltrexone (10 mg/kg) twice daily during gestation and throughout lactation, 21 days postpartum. One, three and seven weeks after birth, male offspring were tested for locomotor activity. At 7 weeks of age, dose-response curves were obtained with morphine (10, 31.6, and 100 mg/kg) and amphetamine (0.31, 10 and 31.6 mg/kg) in naltrexone-pretreated and in saline-treated animals. Naltrexone exposure during gestation and lactation resulted in an augmented sensitivity of offspring to the locomotor activity-increasing effects of morphine. In these animals, the dose-response relationship for the effect of morphine on locomotor activity was displaced to the left about threefold. In contrast, naltrexone exposure did not alter the sensitivity of offspring to amphetamine. It was also found that offspring of naltrexone-treated animals have significantly greater spontaneous locomotor activity than that of the offspring of saline-treated mothers. The increased locomotor activity persisted for at least 4 weeks after the last injection of naltrexone. These findings indicate that chronic opioid receptor blockade during gestation and early postnatal development induces supersensitivity to the locomotor effects of morphine and is associated with long-lasting behavioral alterations.

摘要

在C-57黑小鼠中研究了慢性产前和产后纳曲酮暴露对后代对吗啡运动效应敏感性的影响。在整个妊娠期和哺乳期(产后21天),给怀孕小鼠每天皮下注射(sc)生理盐水(0.1 ml/10 g)或纳曲酮(10 mg/kg)两次。出生后1周、3周和7周,对雄性后代进行运动活性测试。在7周龄时,对纳曲酮预处理和生理盐水处理的动物,用吗啡(10、31.6和100 mg/kg)和苯丙胺(0.31、10和31.6 mg/kg)绘制剂量反应曲线。妊娠期和哺乳期暴露于纳曲酮导致后代对吗啡增加运动活性的效应敏感性增强。在这些动物中,吗啡对运动活性的效应的剂量反应关系向左移位约三倍。相比之下,纳曲酮暴露并未改变后代对苯丙胺的敏感性。还发现,纳曲酮处理动物的后代比生理盐水处理母亲的后代具有明显更高的自发运动活性。在最后一次注射纳曲酮后,增加的运动活性持续至少4周。这些发现表明,妊娠期和产后早期发育期间的慢性阿片受体阻断会诱导对吗啡运动效应的超敏感性,并与长期的行为改变有关。

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