首页> 美国卫生研究院文献>The Journal of Neuroscience >Uncoupling of GABAA/benzodiazepine receptor alpha 1 beta 2 and gamma 2 subunit mRNA expression in cerebellar Purkinje cells of staggerer mutant mice
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Uncoupling of GABAA/benzodiazepine receptor alpha 1 beta 2 and gamma 2 subunit mRNA expression in cerebellar Purkinje cells of staggerer mutant mice

机译:交错突变小鼠小脑浦肯野细胞中GABAA /苯并二氮杂receptor受体α1β2和γ2亚基mRNA表达的解偶联

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摘要

The mammalian GABAA/benzodiazepine (GABAA/BZ) receptor is comprised of several subunit isoforms: alpha 1–6, beta 1–13, gamma 1–3 and delta. In the present studies, the expression of alpha 1, beta 2, and gamma 2 subunit mRNAs was examined in cerebellar Purkinje cells and deep cerebellar neurons of staggerer mutant mice during postnatal development. In control animals, the three subunit mRNAs were present at high density in Purkinje cells which, in adult animals, form a monolayer at the interface of the granule cell and molecular layers. The number of Purkinje cells in the staggerer cerebellar cortex is reduced; the majority of those that remain are retained within the granule cell layer and are unable to receive normal afferent synapses from granule cells. The three subunit mRNAs were ex pressed at similar levels in both staggerer and control Purkinje cells until postnatal day 9. After this time, although the alpha 1 subunit mRNA was maintained at control levels in staggerer Purkinje cells, the expression of beta 2 and gamma 2 subunit mRNAs decreased, and was largely absent by postnatal day 20. The loss of beta 2 and gamma 2 mRNA expression in staggerer was specific to Purkinje cells, since all three mRNAs were present throughout postnatal development in other brain regions, including the deep cerebellar nuclei. The present studies indicate that in cerebellar Purkinje cells, the GABAA/BZ receptor alpha 1, and beta 2, and gamma 2, subunit mRNAs are regulated by distinct mechanisms which are differentially affected by the staggerer mutation.
机译:哺乳动物的GABAA /苯并二氮杂(GABAA / BZ)受体由几种亚基同种型组成:α1-6,β1-31,γ1-3和δ。在本研究中,在出生后发育过程中,检查了交错型突变小鼠的小脑浦肯野细胞和小脑深层神经元中α1,β2和γ2亚基mRNA的表达。在对照动物中,三个亚基mRNA高密度存在于浦肯野细胞中,而成年动物在颗粒细胞和分子层的界面上形成单层。交错小脑皮质中的浦肯野细胞数量减少;剩下的大多数保留在颗粒细胞层中,无法从颗粒细胞接受正常的传入突触。直到出生后第9天,在交错细胞和对照Purkinje细胞中均以相似的水平表达3个亚基的mRNA。此后,尽管在交错动物Purkinje细胞中将α1亚基mRNA维持在对照水平,但beta 2和gamma 2的表达亚基mRNA减少,并在出生后第20天基本消失。交错蛋白中β2和gamma 2 mRNA的表达丢失是浦肯野细胞特有的,因为所有这三种mRNA在整个出生后的整个发育过程中都存在于其他大脑区域,包括小脑深处。 。本研究表明,在小脑浦肯野细胞中,GABAA / BZ受体α1,β2和γ2亚基mRNA受不同机制的调控,这些机制受交错变异的影响不同。

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