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Integrin signalling regulates the expansion of neuroepithelial progenitors and neurogenesis via Wnt7a and Decorin

机译:整合素信号传导通过Wnt7a和Decorin调节神经上皮祖细胞的扩增和神经发生

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Development of the cerebral cortex requires regulation of proliferation and differentiation of neural stem cells and a diverse range of progenitors. Recent work suggests a role for extracellular matrix (ECM) and the major family of ECM receptors, the integrins. Here we show that enhancing integrin beta-1 signalling, by expressing a constitutively active integrin beta-1 (CA*β1) in the embryonic chick mesencephalon, enhances neurogenesis and increases the number of mitotic cells dividing away from the ventricular surface, analogous to sub-apical progenitors in mouse. Only non-integrin-expressing neighbouring cells (lacking CA*β1) contributed to the increased neurogenesis. Transcriptome analysis reveals upregulation of Wnt7a within the CA*β1 cells and upregulation of the ECM protein Decorin in the neighbouring non-expressing cells. Experiments using inhibitors in explant models and genetic knock-downs in vivo reveal an integrin-Wnt7a-Decorin pathway that promotes proliferation and differentiation of neuroepithelial cells, and identify Decorin as a novel neurogenic factor in the central nervous system.
机译:大脑皮层的发育需要调节神经干细胞和各种祖细胞的增殖和分化。最近的工作表明细胞外基质(ECM)和ECM受体的主要家族,整联蛋白的作用。在这里,我们表明,通过在雏鸡中脑中表达组成性活性整联蛋白β-1(CA *β1),增强整联蛋白β-1信号传导,可增强神经发生并增加从心室表面分裂的有丝分裂细胞的数量,类似于亚-小鼠的顶祖细胞。仅非整合素表达的邻近细胞(缺少CA *β1)有助于神经发生的增加。转录组分析揭示CA *β1细胞内Wnt7a的上调和邻近非表达细胞中ECM蛋白Decorin的上调。在外植体模型中使用抑制剂和体内基因敲低的实验表明,整合素-Wnt7a-Decorin途径可促进神经上皮细胞的增殖和分化,并将Decorin鉴定为中枢神经系统中的新型神经源性因子。

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