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lgl, pins and aPKC regulate neuroblast self-renewal versus differentiation

机译:lgl,pin和aPKC调节神经母细胞的自我更新与分化

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How a cell chooses to proliferate or to differentiate is an important issue in stem cell and cancer biology. Drosophila neuroblasts undergo self-renewal with every cell division, producing another neuroblast and a differentiating daughter cell, but the mechanisms controlling the self-renewal/differentiation decision are poorly understood. Here we tested whether cell polarity genes, known to regulate embryonic neuroblast asymmetric cell division(1), also regulate neuroblast self-renewal. Clonal analysis in larval brains showed that pins mutant neuroblasts rapidly fail to self-renew, whereas lethal giant larvae (lgl) mutant neuroblasts generate multiple neuroblasts. Notably, lgl pins double mutant neuroblasts all divide symmetrically to self-renew, filling the brain with neuroblasts at the expense of neurons. The lgl pins neuroblasts show ectopic cortical localization of atypical protein kinase C ( aPKC), and a decrease in aPKC expression reduces neuroblast numbers, suggesting that aPKC promotes neuroblast self-renewal. In support of this hypothesis, neuroblast-specific overexpression of membrane-targeted aPKC, but not a kinase-dead version, induces ectopic neuroblast self-renewal. We conclude that cortical aPKC kinase activity is a potent inducer of neuroblast self-renewal.
机译:细胞如何选择增殖或分化是干细胞和癌症生物学中的重要问题。果蝇神经母细胞每次分裂都会自我更新,产生另一个神经母细胞和一个分化的子细胞,但对自我更新/分化决定的控制机制知之甚少。在这里,我们测试了已知可调节胚胎神经母细胞不对称细胞分裂的细胞极性基因(1)是否也调节了神经母细胞的自我更新。幼虫大脑的克隆分析表明,pin突变型神经母细胞无法快速自我更新,而致死的巨型幼虫(lgl)突变型神经母细胞则产生多个神经母细胞。值得注意的是,lgl销双突变型神经母细胞均对称分裂以自我更新,使神经母细胞充满了神经母细胞,但却损害了神经元。 lgl针神经母细胞显示非典型蛋白激酶C(aPKC)的异位皮层定位,而aPKC表达的减少则减少了神经母细胞的数量,表明aPKC促进了神经母细胞的自我更新。支持该假设的是,针对膜的aPKC的神经母细胞特异性过表达(而不是激酶致死的形式)诱导异位神经母细胞自我更新。我们得出结论,皮质aPKC激酶活性是成神经细胞自我更新的有效诱导剂。

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