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Stabilization of the p53 transformation-related protein in mouse fibrosarcoma cell lines: effects of protein sequence and intracellular environment.

机译:小鼠纤维肉瘤细胞系中p53转化相关蛋白的稳定化:蛋白序列和细胞内环境的影响。

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摘要

The transformation-related protein p53 is normally very labile. The stability of p53 is significantly increased in a number of fibrosarcoma cell lines derived from mouse tumors induced by treatment with physical or chemical agents. In many instances, p53 stabilization is correlated with the ability to form a stable complex with the heat shock protein cognate hsc70. We describe a line in which p53 is very stable yet has no detectable interaction with hsc70. The inability to form such a complex probably resides in the primary structure of the endogenous p53, since introduction of other p53 variants into those cells resulted in the appearance of a p53-hsc70 complex. The factors affecting p53 stability were investigated by stable transfection experiments. The results indicated that the primary structure of the p53 protein is a major determinant of its turnover rate; different p53 variants were degraded at distinct and characteristic rates in a number of transformed cell types. However, at least one p53 variant was degraded differently in nontransformed BALB/c-3T3 than in transformed fibrosarcoma cells, demonstrating that the specific cellular environment can also affect the stability of p53.
机译:转化相关蛋白p53通常非常不稳定。在通过物理或化学试剂治疗诱导的源自小鼠肿瘤的许多纤维肉瘤细胞系中,p53的稳定性显着提高。在许多情况下,p53的稳定与与热激蛋白同源的hsc70形成稳定复合物的能力有关。我们描述了其中p53非常稳定但与hsc70没有可检测的相互作用的品系。不能形成这种复合物的原因可能在于内源性p53的一级结构,因为将其他p53变体引入那些细胞会导致出现p53-hsc70复合物。通过稳定的转染实验研究了影响p53稳定性的因素。结果表明,p53蛋白的一级结构是其周转率的主要决定因素。在许多转化细胞类型中,不同的p53变体以不同的特征速率降解。但是,至少一种p53变体在未转化的BALB / c-3T3中的降解与在转化的纤维肉瘤细胞中的降解不同,这表明特定的细胞环境也可以影响p53的稳定性。

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