Angiopoietin-2 (ANG-2) is a key regulator of angiogenesis that exerts context-dependent effects on ECs. ANG-2 binds the endothelial-specific receptor tyrosine kinase 2 (TIE2) and acts as a negative regulator of ANG-1/TIE2 signaling during angiogenesis, thereby controlling the responsiveness of ECs to exogenous cytokines. Recent data from tumors indicate that under certain conditions ANG-2 can also promote angiogenesis. However, the molecular mechanisms of dual ANG-2 functions are poorly understood. Here, we identify a model for the opposing roles of ANG-2 in angiogenesis. We found that angiogenesis-activated endothelium harbored a subpopulation of TIE2-negative ECs (TIE2lo). TIE2 expression was downregulated in angiogenic ECs, which abundantly expressed several integrins. ANG-2 bound to these integrins in TIE2lo ECs, subsequently inducing, in a TIE2-independent manner, phosphorylation of the integrin adaptor protein FAK, resulting in RAC1 activation, migration, and sprouting angiogenesis. Correspondingly, in vivo ANG-2 blockade interfered with integrin signaling and inhibited FAK phosphorylation and sprouting angiogenesis of TIE2lo ECs. These data establish a contextual model whereby differential TIE2 and integrin expression, binding, and activation control the role of ANG-2 in angiogenesis. The results of this study have immediate translational implications for the therapeutic exploitation of angiopoietin signaling.
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机译:Angiopoietin-2(ANG-2)是血管生成的关键调节剂,对ECs具有上下文相关的作用。 ANG-2结合内皮特异性受体酪氨酸激酶2(TIE2),并在血管生成过程中充当ANG-1 / TIE2信号的负调节剂,从而控制EC对外源细胞因子的响应。来自肿瘤的最新数据表明,在某些条件下,ANG-2也可以促进血管生成。然而,双重ANG-2功能的分子机制了解甚少。在这里,我们确定了ANG-2在血管生成中的相反作用的模型。我们发现,血管生成激活的内皮细胞含有TIE2阴性EC(TIE2 lo )的亚群。 TIE2的表达在血管生成的内皮细胞中被下调,该细胞大量表达多种整合素。 ANG-2在TIE2 lo EC中与这些整合素结合,随后以独立于TIE2的方式诱导整合素衔接蛋白FAK磷酸化,从而导致RAC1活化,迁移和发芽血管生成。相应地,体内ANG-2的阻断会干扰整联蛋白的信号传导,并抑制TIE2 lo EC的FAK磷酸化和发芽血管生成。这些数据建立了上下文模型,其中差异的TIE2和整联蛋白表达,结合和激活控制ANG-2在血管生成中的作用。这项研究的结果对血管生成素信号的治疗开发具有直接的翻译意义。
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