首页> 外文期刊>The European Journal of Neuroscience >Rescue of gamma2 subunit-deficient mice by transgenic overexpression of the GABAA receptor gamma2S or gamma2L subunit isoforms.
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Rescue of gamma2 subunit-deficient mice by transgenic overexpression of the GABAA receptor gamma2S or gamma2L subunit isoforms.

机译:通过转基因过表达GABAA受体gamma2S或gamma2L亚基同种型来拯救gamma2亚基缺陷型小鼠。

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摘要

The gamma2 subunit is an important functional determinant of GABAA receptors and is essential for formation of high-affinity benzodiazepine binding sites and for synaptic clustering of major GABAA receptor subtypes along with gephyrin. There are two splice variants of the gamma2 subunit, gamma2 short (gamma2S) and gamma2 long (gamma2L), the latter carrying in the cytoplasmic domain an additional eight amino acids with a putative phosphorylation site. Here, we show that transgenic mice expressing either the gamma2S or gamma2L subunit on a gamma2 subunit-deficient background are phenotypically indistinguishable from wild-type. They express nearly normal levels of gamma2 subunit protein and [3H]flumazenil binding sites. Likewise, the distribution, number and size of GABAA receptor clusters colocalized with gephyrin are similar to wild-type in both juvenile and adult mice. Our results indicate that the two gamma2 subunit splice variants can substitute for each other and fulfil the basic functions of GABAA receptors, allowing in vivo studies that address isoform-specific roles in phosphorylation-dependent regulatory mechanisms.
机译:γ2亚基是GABAA受体的重要功能决定簇,对于形成高亲和力的苯二氮卓结合位点以及与Gephrin一起形成主要GABAA受体亚型的突触聚簇至关重要。 gamma2亚基有两个剪接变体,即gamma2 short(gamma2S)和gamma2 long(gamma2L),后者在胞质结构域中携带具有推测的磷酸化位点的另外八个氨基酸。在这里,我们显示了在gamma2亚基缺陷背景上表达gamma2S或gamma2L亚基的转基因小鼠在表型上与野生型没有区别。它们表达接近正常水平的gamma2亚基蛋白和[3H]氟马西尼结合位点。同样,在幼年和成年小鼠中,与gephyrin共定位的GABAA受体簇的分布,数量和大小与野生型相似。我们的结果表明,这两个gamma2亚基剪接变体可以彼此替代并完成GABAA受体的基本功能,从而可以进行体内研究,以解决磷酸化依赖性调节机制中的同工型特异性作用。

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