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血管生成素-1对人内皮细胞的直接作用:网络稳定、细胞存活以及与其他血管生成生长因子相互作用的证据

Direct actions of angiopoietin-1 on human endothelium: evidence for network stabilization, cell survival, and interaction with other angiogenic growth factors.

作者信息

Papapetropoulos A, García-Cardeña G, Dengler T J, Maisonpierre P C, Yancopoulos G D, Sessa W C

机构信息

Department of Pharmacology, The Boyer Center for Molecular Medicine, Yale University School of Medicine, New Haven, Connecticut 06536-0812, USA.

出版信息

Lab Invest. 1999 Feb;79(2):213-23.

PMID:10068209
Abstract

Angiopoietin-1 (Ang-1) is a recently described angiogenic protein that activates the endothelial Tie 2 receptor. Disruption of the Ang-1 gene shows that it has an indispensable role in blood vessel development, but it is not clear what specific effects, if any, Ang-1 has on endothelial cell (EC) phenotypes. Here, we show that Ang-1 dose-dependently stabilizes HUVEC network organization for up to 48 hours; this action of Ang-1 is dependent on Tie-2 receptor activation, because a soluble form of the Tie2-, but not the Tie1-receptor, completely blocks the effects of Ang-1. Moreover, we show that Ang-1 potentiates the actions of other angiogenic growth factors. Ang-1 markedly increases the survival of vascular networks (up to 96 hours) exposed to either vascular endothelial growth factor or endothelial cell growth supplement, a form of acidic fibroblast growth factor. In addition, Ang-1 prevents apoptotic death in HUVEC triggered by withdrawal of endothelial cell growth supplement. Collectively, these data are consistent with the idea that Ang-1 directly acts on human EC and interacts with other angiogenic molecules to stabilize vascular structures by promoting the survival of differentiated ECs.

摘要

血管生成素-1(Ang-1)是一种最近被描述的血管生成蛋白,可激活内皮细胞Tie 2受体。Ang-1基因的破坏表明它在血管发育中具有不可或缺的作用,但尚不清楚Ang-1对内皮细胞(EC)表型是否有特定影响(如果有的话)。在这里,我们表明Ang-1以剂量依赖的方式使HUVEC网络组织稳定长达48小时;Ang-1的这种作用依赖于Tie-2受体的激活,因为可溶性形式的Tie2受体(而非Tie1受体)完全阻断了Ang-1的作用。此外,我们表明Ang-1可增强其他血管生成生长因子的作用。Ang-1显著提高了暴露于血管内皮生长因子或内皮细胞生长补充剂(一种酸性成纤维细胞生长因子形式)的血管网络的存活率(长达96小时)。此外,Ang-1可防止因撤除内皮细胞生长补充剂而引发的HUVEC凋亡死亡。总体而言,这些数据与以下观点一致:Ang-1直接作用于人类EC,并与其他血管生成分子相互作用,通过促进分化的EC存活来稳定血管结构。

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