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孕期暴露于CB-1受体激动剂WIN 55212-2或一氧化碳对大鼠小脑皮质GABA能神经元系统的影响。

Effects of prenatal exposure to the CB-1 receptor agonist WIN 55212-2 or CO on the GABAergic neuronal systems of rat cerebellar cortex.

作者信息

Benagiano V, Lorusso L, Flace P, Girolamo F, Rizzi A, Sabatini R, Auteri P, Bosco L, Cagiano R, Ambrosi G

机构信息

Department of Human Anatomy & Histology, Medical Faculty, University of Bari Policlinico, 11 Piazza Giulio Cesare, 70124, Bari, Italy.

出版信息

Neuroscience. 2007 Nov 9;149(3):592-601. doi: 10.1016/j.neuroscience.2007.07.050. Epub 2007 Aug 19.

Abstract

The aim of this study was to assess the effects of prenatal exposures to cannabinoids or carbon monoxide (CO) in an animal experimental model reproducing the environmental conditions in which a fetus develops whose mother, during pregnancy, ingests by smoking low doses of cannabinoids or CO. Particular attention was devoted to analyses of the long-term effects of the exposures at the level of the cerebellar cortex, where already during prenatal development the GABAergic neuronal systems may be modulated by both cannabinoids and CO. Three groups of rats were subjected to the following experimental conditions: exposure to cannabinoids by maternal treatment during pregnancy with the cannabinoid CB-1 receptor agonist WIN 55212-2 (WIN) (0.5 mg/kg/day, s.c.); exposure to CO by maternal exposure during pregnancy to CO (75 parts per million, by inhalation); and exposure to WIN+CO at the above doses and means of administration; a fourth group was used as control. The body weight of dams, length of pregnancy, litter size at birth, body weight and postnatal mortality of pups were monitored in order to evaluate possible effects of the exposures on reproduction and on prenatal and postnatal development. In the different groups, the long-term effects of the exposures were studied in adult rats (120-150 days) by light microscopy analyses of the structure of the cerebellar cortex and of the distribution in the cortex of markers of GABAergic neurons, such as GAD and GABA itself. Results. Exposures to WIN or CO did not affect reproduction or prenatal/postnatal development. Moreover, the exposed rats showed no structural alterations of the cerebellar cortex and displayed qualitative distribution patterns of GAD and GABA immunoreactivities similar to those of the controls. However, quantitative analyses indicated significant changes of both of these immunoreactivities: in comparison with the controls, they were significantly increased in WIN-exposed rats and reduced in CO-exposed rats, but not significantly different in WIN+CO-exposed rats. The changes were detected in the molecular and Purkinje neuron layers, but not in the granular layer. Prenatal exposures of rats to WIN or CO, at doses that do not affect reproduction, general processes of development and histomorphogenesis of the cerebellar cortex, cause significant changes of GAD and GABA immunoreactivities in some GABAergic neuronal systems of the adult rat cerebellar cortex, indicating selective up-regulation of GABA-mediated neurotransmission as a long-term consequence of chronic prenatal exposures to cannabinoids or CO. Because the changes consist of overexpression or, vice versa, underexpression of these immunoreactivities, functional alterations of opposite types in the GABAergic systems of the cerebellum following exposure to WIN or CO can be postulated, in agreement with the results of behavioral and clinical studies. No changes in immunoreactivities were detected after prenatal exposure to WIN and CO in association.

摘要

本研究的目的是在一个动物实验模型中评估产前暴露于大麻素或一氧化碳(CO)的影响,该模型再现了胎儿发育的环境条件,即胎儿的母亲在怀孕期间通过吸烟摄入低剂量的大麻素或CO。特别关注了在小脑皮质水平上暴露的长期影响,在产前发育期间,GABA能神经元系统可能受到大麻素和CO的调节。三组大鼠接受了以下实验条件:在怀孕期间通过母体给予大麻素CB-1受体激动剂WIN 55212-2(WIN)(0.5mg/kg/天,皮下注射)暴露于大麻素;在怀孕期间通过母体吸入CO(百万分之75)暴露于CO;以及以上述剂量和给药方式暴露于WIN+CO;第四组用作对照。监测母鼠的体重、怀孕时长、出生时的窝仔数、幼崽的体重和产后死亡率,以评估暴露对繁殖以及产前和产后发育的可能影响。在不同组中,通过对成年大鼠(120 - 150天)小脑皮质结构以及GABA能神经元标志物(如GAD和GABA本身)在皮质中的分布进行光学显微镜分析,研究暴露的长期影响。结果。暴露于WIN或CO对繁殖或产前/产后发育没有影响。此外,暴露的大鼠小脑皮质没有结构改变,并且GAD和GABA免疫反应性的定性分布模式与对照组相似。然而,定量分析表明这两种免疫反应性都有显著变化:与对照组相比,WIN暴露组大鼠中它们显著增加,CO暴露组大鼠中它们减少,但WIN + CO暴露组大鼠中没有显著差异。这些变化在分子层和浦肯野神经元层中检测到,但在颗粒层中未检测到。大鼠产前暴露于WIN或CO,剂量不影响繁殖、一般发育过程和小脑皮质的组织形态发生,但会导致成年大鼠小脑皮质某些GABA能神经元系统中GAD和GABA免疫反应性的显著变化,表明慢性产前暴露于大麻素或CO的长期后果是GABA介导的神经传递选择性上调。因为这些变化包括这些免疫反应性的过表达或相反的低表达,所以可以假设在暴露于WIN或CO后小脑GABA能系统中会出现相反类型的功能改变,这与行为和临床研究结果一致。产前联合暴露于WIN和CO后未检测到免疫反应性的变化。

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