Fernández Jaime G, Rodríguez Diego A, Valenzuela Manuel, Calderon Claudia, Urzúa Ulises, Munroe David, Rosas Carlos, Lemus David, Díaz Natalia, Wright Mathew C, Leyton Lisette, Tapia Julio C, Quest Andrew Fg
Laboratorio de Comunicaciones Celulares, Centro de Estudios Moleculares de la Célula (CEMC), Programa de Biología Celular y Molecular, ICBM, Facultad de Medicina, Universidad de Chile, Santiago, Chile.
Mol Cancer. 2014 Sep 9;13:209. doi: 10.1186/1476-4598-13-209.
Early in cancer development, tumour cells express vascular endothelial growth factor (VEGF), a secreted molecule that is important in all stages of angiogenesis, an essential process that provides nutrients and oxygen to the nascent tumor and thereby enhances tumor-cell survival and facilitates growth. Survivin, another protein involved in angiogenesis, is strongly expressed in most human cancers, where it promotes tumor survival by reducing apoptosis as well as favoring endothelial cell proliferation and migration. The mechanisms by which cancer cells induce VEGF expression and angiogenesis upon survivin up-regulation remain to be fully established. Since the PI3K/Akt signalling and β-catenin-Tcf/Lef dependent transcription have been implicated in the expression of many cancer-related genes, including survivin and VEGF, we evaluated whether survivin may favor VEGF expression, release from tumor cells and induction of angiogenesis in a PI3K/Akt-β-catenin-Tcf/Lef-dependent manner. Here, we provide evidence linking survivin expression in tumor cells to increased β-catenin protein levels, β-catenin-Tcf/Lef transcriptional activity and expression of several target genes of this pathway, including survivin and VEGF, which accumulates in the culture medium. Alternatively, survivin downregulation reduced β-catenin protein levels and β-catenin-Tcf/Lef transcriptional activity. Also, using inhibitors of PI3K and the expression of dominant negative Akt, we show that survivin acts upstream in an amplification loop to promote VEGF expression. Moreover, survivin knock-down in B16F10 murine melanoma cells diminished the number of blood vessels and reduced VEGF expression in tumors formed in C57BL/6 mice. Finally, in the chick chorioallantoid membrane assay, survivin expression in tumor cells enhanced VEGF liberation and blood vessel formation. Importantly, the presence of neutralizing anti-VEGF antibodies precluded survivin-enhanced angiogenesis in this assay. These findings provide evidence for the existance of a posititve feedback loop connecting survivin expression in tumor cells to PI3K/Akt enhanced β-catenin-Tcf/Lef-dependent transcription followed by secretion of VEGF and angiogenesis.
在癌症发展早期,肿瘤细胞表达血管内皮生长因子(VEGF),这是一种分泌型分子,在血管生成的各个阶段都很重要,血管生成是一个为新生肿瘤提供营养和氧气的关键过程,从而提高肿瘤细胞的存活率并促进其生长。Survivin是另一种参与血管生成的蛋白质,在大多数人类癌症中强烈表达,它通过减少细胞凋亡以及促进内皮细胞增殖和迁移来促进肿瘤存活。癌细胞在Survivin上调后诱导VEGF表达和血管生成的机制仍有待充分阐明。由于PI3K/Akt信号通路和β-连环蛋白-Tcf/Lef依赖性转录与许多癌症相关基因的表达有关,包括Survivin和VEGF,我们评估了Survivin是否可能以PI3K/Akt-β-连环蛋白-Tcf/Lef依赖性方式促进VEGF表达、从肿瘤细胞释放以及诱导血管生成。在此,我们提供证据表明肿瘤细胞中Survivin的表达与β-连环蛋白蛋白水平增加、β-连环蛋白-Tcf/Lef转录活性以及该通路的几个靶基因的表达有关,包括Survivin和VEGF,它们在培养基中积累。相反,Survivin下调降低了β-连环蛋白蛋白水平和β-连环蛋白-Tcf/Lef转录活性。此外,使用PI3K抑制剂和显性负性Akt的表达,我们表明Survivin在一个放大环中起上游作用以促进VEGF表达。此外,B16F10小鼠黑色素瘤细胞中Survivin的敲低减少了C57BL/6小鼠形成的肿瘤中的血管数量并降低了VEGF表达。最后,在鸡胚绒毛尿囊膜试验中,肿瘤细胞中Survivin的表达增强了VEGF释放和血管形成。重要的是,在该试验中,中和性抗VEGF抗体的存在排除了Survivin增强的血管生成。这些发现为存在一个将肿瘤细胞中Survivin表达与PI3K/Akt增强的β-连环蛋白-Tcf/Lef依赖性转录、随后VEGF分泌和血管生成相联系的正反馈环提供了证据。
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