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Evolutionarily conserved anterior expansion of the central nervous system promoted by a common PcG-Hox program

机译:通过普通PCG-HOX计划促进的中枢神经系统的进化保护前膨胀

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A conserved feature of the central nervous system (CNS) is the prominent expansion of anterior regions (brain) compared with posterior (nerve cord). The cellular and regulatory processes driving anterior CNS expansion are not well understood in any bilaterian species. Here, we address this expansion in Drosophila and mouse. We find that, compared with the nerve cord, the brain displays extended progenitor proliferation, more elaborate daughter cell proliferation and more rapid cell cycle speed in both Drosophila and mouse. These features contribute to anterior CNS expansion in both species. With respect to genetic control, enhanced brain proliferation is severely reduced by ectopic Hox gene expression, by either Hox misexpression or by loss of Polycomb group (PcG) function. Strikingly, in PcG mutants, early CNS proliferation appears to be unaffected, whereas subsequent brain proliferation is severely reduced. Hence, a conserved PcG-Hox program promotes the anterior expansion of the CNS. The profound differences in proliferation and in the underlying genetic mechanisms between brain and nerve cord lend support to the emerging concept of separate evolutionary origins of these two CNS regions.
机译:中枢神经系统(CNS)的保守特征是与后部(神经帘线)相比的前部区域(脑)的突出膨胀。在任何双玻璃种类中,驾驶前CNS扩增的细胞和调节过程尚未得到很好的理解。在这里,我们在果蝇和鼠标中解决了这种扩张。我们发现,与神经脐带相比,大脑显示出延长的祖细胞增殖,更精细的子细胞增殖和更快速的细胞周期速度在果蝇和小鼠中。这些功能有助于两种物种中的前CNS扩展。关于遗传控制,通过霍克斯MiseSx抑制或通过损失多功能组织(PCG)功能,通过异位HOX基因表达严重减少增强的脑增殖。在PCG突变体中引人注目,早期的CNS增殖似乎不受影响,而随后的脑增殖严重降低。因此,保守的PCG-HOX计划促进了CNS的前膨胀。扩散的深刻差异以及脑和神经线之间的潜在遗传机制对这两个CNS区域的单独进化起源的新兴概念。

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