Molecular Biology Institute, University of California at Los Angeles, CA 90095, USA.
Genes Dev. 2012 Mar 1;26(5):445-60. doi: 10.1101/gad.182477.111. Epub 2012 Feb 22.
The Rbfox proteins (Rbfox1, Rbfox2, and Rbfox3) regulate the alternative splicing of many important neuronal transcripts and have been implicated in a variety of neurological disorders. However, their roles in brain development and function are not well understood, in part due to redundancy in their activities. Here we show that, unlike Rbfox1 deletion, the CNS-specific deletion of Rbfox2 disrupts cerebellar development. Genome-wide analysis of Rbfox2(-/-) brain RNA identifies numerous splicing changes altering proteins important both for brain development and mature neuronal function. To separate developmental defects from alterations in the physiology of mature cells, Rbfox1 and Rbfox2 were deleted from mature Purkinje cells, resulting in highly irregular firing. Notably, the Scn8a mRNA encoding the Na(v)1.6 sodium channel, a key mediator of Purkinje cell pacemaking, is improperly spliced in RbFox2 and Rbfox1 mutant brains, leading to highly reduced protein expression. Thus, Rbfox2 protein controls a post-transcriptional program required for proper brain development. Rbfox2 is subsequently required with Rbfox1 to maintain mature neuronal physiology, specifically Purkinje cell pacemaking, through their shared control of sodium channel transcript splicing.
Rbfox 蛋白(Rbfox1、Rbfox2 和 Rbfox3)调节许多重要神经元转录本的可变剪接,并且与多种神经疾病有关。然而,它们在大脑发育和功能中的作用还不是很清楚,部分原因是它们的活性存在冗余。在这里,我们发现,与 Rbfox1 缺失不同,Rbfox2 的中枢神经系统特异性缺失会破坏小脑发育。对 Rbfox2(-/-)大脑 RNA 的全基因组分析确定了许多剪接变化,这些变化改变了对大脑发育和成熟神经元功能都很重要的蛋白质。为了将发育缺陷与成熟细胞的生理学改变分开,我们从成熟的浦肯野细胞中删除了 Rbfox1 和 Rbfox2,导致高度不规则的放电。值得注意的是,编码 Na(v)1.6 钠通道的 Scn8a mRNA 在 RbFox2 和 Rbfox1 突变体大脑中被不正确剪接,导致蛋白表达水平显著降低。因此,Rbfox2 蛋白控制着一个转录后程序,对于正常的大脑发育是必需的。随后,Rbfox2 与 Rbfox1 一起维持成熟神经元的生理学,特别是浦肯野细胞的起搏,通过它们对钠通道转录本剪接的共同控制。
