Current models of brain development support the view that VEGF, a signaling protein secreted by neuronal cells, regulates angiogenesis and neuronal development. Here we demonstrate an autonomous and pivotal role for endothelial cell-derived VEGF that has far-reaching consequences for mouse brain development. Selective deletion of Vegf from endothelial cells resulted in impaired angiogenesis and marked perturbation of cortical cytoarchitecture. Abnormal cell clusters or heterotopias were detected in the marginal zone, and disorganization of cortical cells induced several malformations, including aberrant cortical lamination. Critical events during brain development-neuronal proliferation, differentiation, and migration were significantly affected. In addition, axonal tracts in the telencephalon were severely defective in the absence of endothelial VEGF. The unique roles of endothelial VEGF cannot be compensated by neuronal VEGF and underscores the high functional significance of endothelial VEGF for cerebral cortex development and from disease perspectives.

译文

目前的大脑发育模型支持以下观点: VEGF是神经元细胞分泌的信号蛋白,可调节血管生成和神经元发育。在这里,我们证明了内皮细胞衍生的VEGF的自主和关键作用,对小鼠大脑发育具有深远的影响。内皮细胞中Vegf的选择性缺失导致血管生成受损和皮质细胞结构的明显扰动。在边缘区检测到异常的细胞簇或异型,皮质细胞的紊乱引起了几种畸形,包括异常的皮质层合。大脑发育过程中的关键事件-神经元增殖,分化和迁移受到显着影响。此外,在没有内皮VEGF的情况下,端脑中的轴突束严重缺陷。内皮VEGF的独特作用不能通过神经元VEGF来补偿,并从疾病的角度强调了内皮VEGF对大脑皮层发育的高度功能意义。

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