Chen Lei, Melendez Jaime, Campbell Kenneth, Kuan Chia-Yi, Zheng Yi
Divisios of Experimental Hematology, University of Cincinnati, Cincinnati, OH 45229, USA.
Dev Biol. 2009 Jan 1;325(1):162-70. doi: 10.1016/j.ydbio.2008.10.023. Epub 2008 Oct 31.
The Rho family of small GTPases has been implicated in many neurological disorders including mental retardation, but whether they are involved in primary microcephaly (microcephalia vera) is unknown. Here, we examine the role of Rac1 in mammalian neural progenitors and forebrain development by a conditional gene-targeting strategy using the Foxg1-Cre line to delete floxed-Rac1 alleles in the telencephalic ventricular zone (VZ) of mouse embryos. We found that Rac1 deletion in the telencephalic VZ progenitors resulted in reduced sizes of both the striatum and cerebral cortex. Analyses further indicated that this abnormality was caused by accelerated cell-cycle exit and increased apoptosis during early corticogenesis (approximately E14.5), leading to a decrease of the neural progenitor pool in mid-to-late telencephalic development (E16.5 to E18.5). Moreover, the formation of patch-matrix compartments in the striatum was impaired by Rac1-deficiency. Together, these results suggest that Rac1 regulates self-renewal, survival, and differentiation of telencephalic neural progenitors, and that dysfunctions of Rac1 may lead to primary microcephaly.
小GTP酶的Rho家族与包括智力迟钝在内的许多神经疾病有关,但它们是否参与原发性小头畸形(真性小头畸形)尚不清楚。在这里,我们通过条件基因靶向策略,利用Foxg1-Cre系在小鼠胚胎的端脑室管膜区(VZ)中删除floxed-Rac1等位基因,来研究Rac1在哺乳动物神经祖细胞和前脑发育中的作用。我们发现,端脑室管膜区祖细胞中Rac1的缺失导致纹状体和大脑皮层的大小减小。进一步分析表明,这种异常是由早期皮质发生过程中(约E14.5)细胞周期退出加速和细胞凋亡增加引起的,导致端脑发育中后期(E16.5至E18.5)神经祖细胞池减少。此外,Rac1缺陷会损害纹状体中斑块-基质区室的形成。总之,这些结果表明Rac1调节端脑神经祖细胞的自我更新、存活和分化,并且Rac1功能障碍可能导致原发性小头畸形。
