Damalas A, Ben-Ze'ev A, Simcha I, Shtutman M, Leal J F, Zhurinsky J, Geiger B, Oren M
Department of Molecular Cell Biology, The Weizmann Institute of Science, Rehovot 76100, Israel.
EMBO J. 1999 Jun 1;18(11):3054-63. doi: 10.1093/emboj/18.11.3054.
beta-catenin is a multifunctional protein, acting both as a structural component of the cell adhesion machinery and as a transducer of extracellular signals. Deregulated beta-catenin protein expression, due to mutations in the beta-catenin gene itself or in its upstream regulator, the adenomatous polyposis coli (APC) gene, is prevalent in colorectal cancer and in several other tumor types, and attests to the potential oncogenic activity of this protein. Increased expression of beta-catenin is an early event in colorectal carcinogenesis, and is usually followed by a later mutational inactivation of the p53 tumor suppressor. To examine whether these two key steps in carcinogenesis are interrelated, we studied the effect of excess beta-catenin on p53. We report here that overexpression of beta-catenin results in accumulation of p53, apparently through interference with its proteolytic degradation. This effect involves both Mdm2-dependent and -independent p53 degradation pathways, and is accompanied by augmented transcriptional activity of p53 in the affected cells. Increased p53 activity may provide a safeguard against oncogenic deregulation of beta-catenin, and thus impose a pressure for mutational inactivation of p53 during the later stages of tumor progression.
β-连环蛋白是一种多功能蛋白质,既是细胞黏附机制的结构成分,又是细胞外信号的转导分子。由于β-连环蛋白基因本身或其上游调节因子腺瘤性息肉病大肠杆菌(APC)基因发生突变,导致β-连环蛋白蛋白表达失调,在结直肠癌和其他几种肿瘤类型中很常见,这证明了该蛋白潜在的致癌活性。β-连环蛋白表达增加是结直肠癌发生的早期事件,通常随后会出现p53肿瘤抑制因子的后期突变失活。为了研究致癌过程中的这两个关键步骤是否相互关联,我们研究了过量β-连环蛋白对p53的影响。我们在此报告,β-连环蛋白的过表达导致p53积累,显然是通过干扰其蛋白水解降解。这种效应涉及依赖Mdm2和不依赖Mdm2的p53降解途径,并且在受影响的细胞中伴随着p53转录活性的增强。p53活性增加可能对β-连环蛋白的致癌失调起到保护作用,从而在肿瘤进展的后期对p53的突变失活施加压力。