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禽血管内皮生长因子-C:克隆、胚胎表达模式及对表达血管内皮生长因子受体2的内皮细胞前体分化的刺激作用

Avian VEGF-C: cloning, embryonic expression pattern and stimulation of the differentiation of VEGFR2-expressing endothelial cell precursors.

作者信息

Eichmann A, Corbel C, Jaffredo T, Bréant C, Joukov V, Kumar V, Alitalo K, le Douarin N M

机构信息

Institut d'Embryologie Cellulaire et Moléculaire du CNRS et du Collège de France, Nogent-sur-Marne, France.

出版信息

Development. 1998 Feb;125(4):743-52. doi: 10.1242/dev.125.4.743.

Abstract

VEGF-C is a recently discovered secreted polypeptide related to the angiogenic mitogen VEGF. We have isolated the quail VEGF-C cDNA and shown that its protein product is secreted from transfected cells and interacts with the avian VEGFR3 and VEGFR2. In situ hybridization shows that quail VEGF-C mRNA is strongly expressed in regions destined to be rich in lymphatic vessels, particularly the mesenteries, mesocardium and myotome, in the region surrounding the jugular veins, and in the kidney. These expression sites are similar to those observed in the mouse embryo (E. Kukk, A. Lymboussaki, S. Taira, A. Kaipainen, M. Jeltsch, V. Joukov and K. Alitalo, 1996, Development 122, 3829-3837). We have observed VEGFR3-positive endothelial cells in proximity to most of the VEGF-C-expressing sites, suggesting functional relationships between this receptor-ligand couple. The comparison of the VEGF and VEGFR2 knockout phenotypes had suggested the existence of another ligand for VEGFR2. We therefore investigated the effect of VEGF-C on VEGFR2-positive cells isolated from the posterior mesoderm of gastrulating embryos. We have recently shown that VEGF binding triggers endothelial differentiation of these cells, whereas hemopoietic differentiation appears to be mediated by binding of a so far unidentified VEGFR2 ligand. We show here that VEGF-C also triggers endothelial differentiation of these cells, presumably via VEGFR2. These results indicate that VEGF and VEGF-C can act in a redundant manner via VEGFR2. In conclusion, VEGF-C appears to act during two different developmental phases, one early in posterior mesodermal VEGFR2-positive endothelial cell precursors which are negative for VEGFR3 and one later in regions rich in lymphatic vessels at a time when endothelial cells express both VEGFR2 and VEGFR3.

摘要

血管内皮生长因子C(VEGF-C)是最近发现的一种与血管生成有丝分裂原VEGF相关的分泌型多肽。我们已经分离出鹌鹑VEGF-C的互补DNA(cDNA),并表明其蛋白质产物可从转染细胞中分泌出来,并与禽血管内皮生长因子受体3(VEGFR3)和血管内皮生长因子受体2(VEGFR2)相互作用。原位杂交显示,鹌鹑VEGF-C信使核糖核酸(mRNA)在注定富含淋巴管的区域强烈表达,特别是肠系膜、心系膜和肌节,颈静脉周围区域以及肾脏。这些表达位点与在小鼠胚胎中观察到的相似(E. Kukk、A. Lymboussaki、S. Taira、A. Kaipainen、M. Jeltsch、V. Joukov和K. Alitalo,1996年,《发育》122卷,3829 - 3837页)。我们在大多数VEGF-C表达位点附近观察到VEGFR3阳性内皮细胞,这表明该受体 - 配体对之间存在功能关系。VEGF和VEGFR2基因敲除表型的比较表明存在VEGFR2的另一种配体。因此,我们研究了VEGF-C对从原肠胚后中胚层分离出的VEGFR2阳性细胞的影响。我们最近表明,VEGF结合可触发这些细胞的内皮分化,而造血分化似乎是由一种迄今未鉴定的VEGFR2配体的结合介导的。我们在此表明,VEGF-C也可触发这些细胞的内皮分化,推测是通过VEGFR2。这些结果表明,VEGF和VEGF-C可通过VEGFR2以冗余方式发挥作用。总之,VEGF-C似乎在两个不同的发育阶段发挥作用,一个阶段是在VEGFR3阴性的后中胚层VEGFR2阳性内皮细胞前体的早期,另一个阶段是在富含淋巴管的区域后期,此时内皮细胞同时表达VEGFR2和VEGFR3。

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