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Spatial regulation of VEGF receptor endocytosis in angiogenesis

机译:血管生成中VEGF受体内吞的空间调节

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Activities as diverse as migration, proliferation and patterning occur simultaneously and in a coordinated fashion during tissue morphogenesis. In the growing vasculature, the formation of motile, invasive and filopodia-carrying endothelial sprouts is balanced with the stabilization of blood-transporting vessels. Here, we show that sprouting endothelial cells in the retina have high rates of VEGF uptake, VEGF receptor endocytosis and turnover. These internalization processes are opposed by atypical protein kinase C activity in more stable and mature vessels. aPKC phosphorylates Dab2, a clathrin-associated sorting protein that, together with the transmembrane protein ephrin-B2 and the cell polarity regulator PAR-3, enables VEGF receptor endocytosis and downstream signal transduction. Accordingly, VEGF receptor internalization and the angiogenic growth of vascular beds are defective in loss-of-function mice lacking key components of this regulatory pathway. Our work uncovers how vessel growth is dynamically controlled by local VEGF receptor endocytosis and the activity of cell polarity proteins.
机译:在组织形态发生过程中,以协调一致的方式同时发生迁移,增殖和构图等多种活动。在不断增长的脉管系统中,运动的,侵袭性的和携带丝状伪足的内皮新芽的形成与输血血管的稳定相平衡。在这里,我们显示视网膜中发芽的内皮细胞具有较高的VEGF摄取率,VEGF受体内吞作用和周转率。这些内在化过程与更稳定和成熟的血管中的非典型蛋白激酶C活性相反。 aPKC使网格蛋白相关的分选蛋白Dab2磷酸化,并与跨膜蛋白ephrin-B2和细胞极性调节剂PAR-3一起使VEGF受体内吞和下游信号转导。因此,在缺乏该调节途径的关键成分的功能丧失的小鼠中,VEGF受体内在化和血管床的血管生成生长是有缺陷的。我们的工作揭示了局部VEGF受体内吞作用和细胞极性蛋白的活性如何动态地控制血管的生长。

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