An in vivo function for the transforming Myc protein: elicitation of the angiogenic phenotype.

C V Ngo, M Gee, N Akhtar, D Yu, O Volpert, R Auerbach, A Thomas-Tikhonenko
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Abstract

The ability of neoplastic cells to recruit blood vasculature is crucial to their survival in the host organism. However, the evidence linking dominant oncogenes to the angiogenic switch remains incomplete. We demonstrate here that Myc, an oncoprotein implicated in many human malignancies, stimulates neovascularization. As an experimental model, we used Rat-1A fibroblasts that form vascular tumors upon transformation by Myc in immunocompromised mice. Our previous work and the use of neutralizing antibodies reveal that in these cells, the angiogenic switch is achieved via down-modulation of thrombospondin-1, a secreted inhibitor of angiogenesis, whereas the levels of vascular endothelial growth factor, a major activator of angiogenesis, remain high and unaffected by Myc. Consistent with this finding, overexpression of Myc confers upon the conditioned media the ability to promote migration of adjacent endothelial cells in vitro and corneal neovascularization in vivo. Furthermore, mobilization of estrogen-dependent Myc in vivo with the appropriate steroid provokes neovascularization of cell implants embedded in Matrigel. These data suggest that Myc is fully competent to trigger the angiogenic switch in vivo and that secondary events may not be required for neovascularization of Myc-induced tumors.

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转化Myc蛋白的体内功能:引发血管生成表型。
肿瘤细胞招募血管的能力对它们在宿主体内的生存至关重要。然而,将显性癌基因与血管生成开关联系起来的证据仍然不完整。我们在这里证明了Myc,一种与许多人类恶性肿瘤有关的癌蛋白,可以刺激新生血管。作为实验模型,我们使用了免疫功能低下小鼠经Myc转化后形成血管肿瘤的大鼠- 1a成纤维细胞。我们之前的工作和中和抗体的使用表明,在这些细胞中,血管生成开关是通过下调血小板反应蛋白-1(一种血管生成的分泌抑制剂)来实现的,而血管生成的主要激活因子血管内皮生长因子的水平保持高水平,不受Myc的影响。与这一发现一致,Myc的过表达赋予条件培养基在体外促进邻近内皮细胞迁移和体内角膜新生血管形成的能力。此外,体内雌激素依赖性Myc与适当的类固醇的动员可促进嵌入Matrigel的细胞植入物的新生血管形成。这些数据表明,Myc完全有能力在体内触发血管生成开关,Myc诱导的肿瘤新生血管可能不需要继发性事件。
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