Keidar Liraz, Gerlitz Gabi, Kshirsagar Aditya, Tsoory Michael, Olender Tsviya, Wang Xing, Yang Ying, Chen Yu-Sheng, Yang Yun-Gui, Voineagu Irina, Reiner Orly
Department of Molecular Genetics, Weizmann Institute of Science, Rehovot, Israel.
Department of Veterinary Resources, Weizmann Institute of Science, Rehovot, Israel.
Front Cell Neurosci. 2019 Aug 14;13:370. doi: 10.3389/fncel.2019.00370. eCollection 2019.
is the main causative gene for lissencephaly, while is the main causative gene for Rett syndrome, both of which are neurodevelopmental diseases. Here we report nuclear functions for LIS1 and identify previously unrecognized physical and genetic interactions between the products of these two genes in the cell nucleus, that has implications on MeCP2 organization, neuronal gene expression and mouse behavior. Reduced LIS1 levels affect the association of MeCP2 with chromatin. Transcriptome analysis of primary cortical neurons derived from wild type, ±, , or double mutants mice revealed a large overlap in the differentially expressed (DE) genes between the various mutants. Overall, our findings provide insights on molecular mechanisms involved in the neurodevelopmental disorders lissencephaly and Rett syndrome caused by dysfunction of LIS1 and MeCP2, respectively.
是无脑回畸形的主要致病基因,而 是雷特综合征的主要致病基因,这两种都是神经发育疾病。在此我们报告了LIS1的核功能,并确定了这两个基因的产物在细胞核中以前未被认识的物理和遗传相互作用,这对MeCP2的组织、神经元基因表达和小鼠行为有影响。LIS1水平降低会影响MeCP2与染色质的结合。对来自野生型、±、 或双突变小鼠的原代皮质神经元进行转录组分析,发现在各种突变体之间差异表达(DE)基因有很大重叠。总体而言,我们的研究结果为分别由LIS1和MeCP2功能障碍引起的神经发育障碍无脑回畸形和雷特综合征所涉及的分子机制提供了见解。
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