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Multiple lineages enable robust development of the neuropil-glia architecture in adult Drosophila

机译:多种谱系能够在成人果蝇中的神经覆盖胶型建筑的强大开发

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摘要

Neural remodeling is essential for the development of a functional nervous system and has been extensively studied in the metamorphosis of Drosophila. Despite the crucial roles of glial cells in brain functions, including learning and behavior, little is known of how adult glial cells develop in the context of neural remodeling. Here, we show that the architecture of neuropil-glia in the adult Drosophila brain, which is composed of astrocyte-like glia (ALG) and ensheathing glia (EG), robustly develops from two different populations in the larva: the larval EG and glial cell missing-positive (gcm(+)) cells. Whereas gcm(+) cells proliferate and generate adult ALG and EG, larval EG dedifferentiate, proliferate and redifferentiate into the same glial subtypes. Each glial lineage occupies a certain brain area complementary to the other, and together they form the adult neuropil-glia architecture. Both lineages require the FGF receptor Heartless to proliferate, and the homeoprotein Prospero to differentiate into ALG. Lineage-specific inhibition of gliogenesis revealed that each lineage compensates for deficiency in the proliferation of the other. Together, the lineages ensure the robust development of adult neuropil-glia, thereby ensuring a functional brain.
机译:神经重塑对于功能性神经系统的发展至关重要,并且在果蝇的变态中被广泛研究。尽管胶质细胞在大脑功能中的角色,包括学习和行为,但众所周知成年胶质细胞在神经重塑的背景下发展。在这里,我们表明,成年果蝇脑中神经毛利胶质的结构,它由白胶质细胞样胶质细胞(ALG)和鞘胶(例如)组成,从幼虫中的两种不同群体中强大地发展:幼虫(例如侏儒)细胞缺失阳性(GCM(+))细胞。而GCM(+)细胞增殖和产生成人ALG,例如幼虫,例如去除了,增殖和再分析成相同的胶质亚型。每个胶质血统占据一定的大脑区域,互补地区,它们在一起形成成人神经胶质彩色架构。两种谱系都需要FGF受体无情地增殖,以及级蛋白蛋白Prospero区分ALG。特异性血管生成的抑制揭示了各种谱系补偿了另一个缺陷的缺陷。在一起,谱系确保了成年神经胶质胶质胶质的稳健发展,从而确保了功能性脑。

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