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首页> 外文期刊>Blood: The Journal of the American Society of Hematology >Identification and functional analysis of endothelial tip cell-enriched genes.
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Identification and functional analysis of endothelial tip cell-enriched genes.

机译:内皮尖细胞富集基因的鉴定和功能分析。

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摘要

Sprouting of developing blood vessels is mediated by specialized motile endothelial cells localized at the tips of growing capillaries. Following behind the tip cells, endothelial stalk cells form the capillary lumen and proliferate. Expression of the Notch ligand Delta-like-4 (Dll4) in tip cells suppresses tip cell fate in neighboring stalk cells via Notch signaling. In DLL4(+/-) mouse mutants, most retinal endothelial cells display morphologic features of tip cells. We hypothesized that these mouse mutants could be used to isolate tip cells and so to determine their genetic repertoire. Using transcriptome analysis of retinal endothelial cells isolated from DLL4(+/-) and wild-type mice, we identified 3 clusters of tip cell-enriched genes, encoding extracellular matrix degrading enzymes, basement membrane components, and secreted molecules. Secreted molecules endothelial-specific molecule 1, angiopoietin 2, and apelin bind to cognate receptors on endothelial stalk cells. Knockout mice and zebrafish morpholino knockdown of apelin showed delayed angiogenesis and reduced proliferation of stalk cells expressing the apelin receptor APJ. Thus, tip cells may regulate angiogenesis via matrix remodeling, production of basement membrane, and release of secreted molecules, some of which regulate stalk cell behavior.
机译:发育中的血管发芽由位于生长的毛细血管尖端的专门的运动性内皮细胞介导。在尖端细胞之后,内皮茎细胞形成毛细血管腔并增殖。 Notch配体Delta-like-4(Dll4)在尖端细胞中的表达可通过Notch信号抑制邻近茎细胞中的尖端细胞命运。在DLL4(+/-)小鼠突变体中,大多数视网膜内皮细胞显示出尖端细胞的形态特征。我们假设这些小鼠突变体可用于分离尖端细胞,从而确定其遗传库。使用从DLL4(+/-)和野生型小鼠分离的视网膜内皮细胞的转录组分析,我们确定了3个尖端细胞富集基因簇,它们编码细胞外基质降解酶,基底膜成分和分泌的分子。分泌的分子内皮特异性分子1,血管生成素2和apelin与内皮柄细胞上的同源受体结合。敲除小鼠和斑马鱼吗啡敲除阿佩林显示延迟的血管生成和减少表达阿佩林受体APJ的茎细胞的增殖。因此,尖端细胞可通过基质重塑,基底膜的产生和分泌分子的释放来调节血管生成,其中一些调节茎细胞的行为。

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