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在患有遗传性癫痫的沙鼠黑质网状部中,GABAA受体介导的抑制性突触后电流和α1亚基表达并未降低。

GABAA receptor-mediated IPSCs and alpha1 subunit expression are not reduced in the substantia nigra pars reticulata of gerbils with inherited epilepsy.

作者信息

Kumar Sanjay S, Wen Xiling, Yang Yufeng, Buckmaster Paul S

机构信息

Department of Comparative Medicine, Stanford University, Stanford, CA 94305-5342, USA.

出版信息

J Neurophysiol. 2006 Apr;95(4):2446-55. doi: 10.1152/jn.01173.2005. Epub 2006 Jan 11.

Abstract

Domestic Mongolian gerbils, a model of inherited epilepsy, begin having spontaneous seizures at approximately 1.5 mo of age, making it possible to evaluate them during epileptic and pre-epileptic stages. Previous studies have shown that GABA binding is reduced in the substantia nigra pars reticulata (SNr) of both epileptic and pre-epileptic gerbils compared with controls, suggesting that reduced expression of GABAA receptors in SNr might be epileptogenic in this model. To test this hypothesis, we measured the expression of the GABAA receptor alpha1 subunit, the dominant alpha subunit expressed in the SNr, and evaluated GABAA receptor-mediated postsynaptic currents in SNr neurons. GABA(A) alpha1 subunit mRNA levels in substantia nigra-rich tissue from pre-epileptic animals were similar to controls, and immunocytochemistry for the alpha1 subunit showed similar strong expression in the SNr in both groups. Western analysis confirmed that expression of the alpha1 subunit protein was similar in substantia nigra-rich tissue from pre-epileptic and control gerbils. The frequency and amplitude of spontaneous inhibitory postsynaptic currents (IPSCs) and the frequency of miniature (m)IPSCs in SNr neurons of pre-epileptic gerbil were similar to those of controls. The amplitude of mIPSCs in the pre-epileptics was significantly larger than controls. Zolpidem, an alpha1 subunit-specific modulator of the GABAA receptor, was equally efficacious in prolonging the decay time of mIPSCs in both groups. Hence, contrary to the predictions of the hypothesis, mRNA and protein expression levels of the major GABAA receptor alpha subunit were normal, and neurons of the SNr in pre-epileptic gerbils displayed normal or enhanced IPSC frequencies and amplitudes. Therefore reduced expression of GABAA receptors in SNr is not likely to be an epileptogenic mechanism in this model.

摘要

蒙古沙土鼠是遗传性癫痫的一种模型,大约在1.5月龄时开始出现自发性癫痫发作,这使得在癫痫发作期和癫痫发作前期对其进行评估成为可能。先前的研究表明,与对照组相比,癫痫发作期和癫痫发作前期的沙土鼠黑质网状部(SNr)中GABA结合减少,这表明SNr中GABAA受体表达降低可能是该模型中的致痫原因。为了验证这一假设,我们测量了SNr中主要表达的GABAA受体α1亚基的表达,并评估了SNr神经元中GABAA受体介导的突触后电流。癫痫发作前期动物富含黑质的组织中GABA(A)α1亚基mRNA水平与对照组相似,α1亚基的免疫细胞化学显示两组SNr中均有相似的强表达。蛋白质印迹分析证实,癫痫发作前期和对照沙土鼠富含黑质的组织中α1亚基蛋白的表达相似。癫痫发作前期沙土鼠SNr神经元中自发性抑制性突触后电流(IPSCs)的频率和幅度以及微小(m)IPSCs的频率与对照组相似。癫痫发作前期的mIPSCs幅度显著大于对照组。唑吡坦是一种GABAA受体α1亚基特异性调节剂,在延长两组mIPSCs的衰减时间方面同样有效。因此,与该假设的预测相反,主要GABAA受体α亚基的mRNA和蛋白表达水平正常,癫痫发作前期沙土鼠的SNr神经元显示出正常或增强的IPSC频率和幅度。因此,SNr中GABAA受体表达降低不太可能是该模型中的致痫机制。

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