The tumor suppressor gene, p53, is rarely mutated in neuroblastomas (NB) at the time of diagnosis, but its dysfunction could result from a nonfunctional conformation or cytoplasmic sequestration of the wild-type p53 protein. However, p53 mutation, when it occurs, is found in NB tumors with drug resistance acquired over the course of chemotherapy. As yet, no study has been devoted to the function of the specific p53 mutants identified in NB cells. This study includes characterization and functional analysis of p53 expressed in eight cell lines: three wild-type cell lines and five cell lines harboring mutations. We identified two transcription-inactive p53 variants truncated in the C-terminus, one of which corresponded to the p53β isoform recently identified in normal tissue by Bourdon et al. [J. C. Bourdon, K. Fernandes, F. Murray-Zmijewski, G. Liu, A. Diot, D. P. Xirodimas, M. K. Saville and D. P. Lane (2005) Genes Dev., 19, 2122–2137]. Our results show, for the first time, that the p53β isoform is the only p53 species to be endogenously expressed in the human NB cell line SK-N-AS, suggesting that the C-terminus truncated p53 isoforms may play an important role in NB tumor development.
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机译:诊断时,抑癌基因p53在神经母细胞瘤(NB)中很少发生突变,但其功能障碍可能是由于野生型p53蛋白的无功能构象或细胞质隔离所致。但是,在NB肿瘤中发现p53突变发生时,其耐药性是在化疗过程中获得的。迄今为止,还没有研究致力于在NB细胞中鉴定出的特定p53突变体的功能。这项研究包括在8种细胞系中表达的p53的表征和功能分析:3种野生型细胞系和5种具有突变的细胞系。我们鉴定了两个在C末端被截短的转录失活的p53变异体,其中之一对应于Bourdon等人最近在正常组织中鉴定出的p53β同工型。 [J. C. Bourdon,K。Fernandes,F。Murray-Zmijewski,G。Liu,A。Diot,D.P。Xirodimas,M。K. Saville和D.P. Lane(2005)Genes Dev。,19,2122–2137]。我们的结果首次显示,p53β亚型是人类NB细胞系SK-N-AS中唯一内源表达的p53物种,这表明C末端截短的p53亚型可能在NB中起重要作用。肿瘤发展。
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