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BMC Cancer  2011 

Limited importance of the dominant-negative effect of TP53 missense mutations

DOI: 10.1186/1471-2407-11-243

Keywords: TP53, heterozygous mutation, dominant-negative effect, cancer cell lines

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Abstract:

Genetic analyses (LOH and sequencing) performed for early and late passages of several cell lines originally described as showing single heterozygous TP53 mutations (H-318, G-16, PF-382, MOLT-13, ST-486 and LS-123). Statistical analysis of IARC TP53 and SANGER databases. Genetic analyses of N-RAS, FBXW7, PTEN and STR markers to test cross-contamination and cell line identity. Cell cloning, fluorescence-activated cell sorting and SSCP performed for the PF-382 cell line.A database study revealed TP53 single heterozygous mutations in 35% of in vivo (surgical and biopsy) samples and only 10% of cultured cells (in vitro), although those numbers appeared to be overestimated. We deem that published in vivo TP53 mutation analyses are not as rigorous as studies in vitro, and we did not find any cell line showing a stable, single heterozygous mutation. G16, PF-382 and MOLT-13 cells harboured single heterozygous mutations temporarily. ST-486, H-318 and LS-123 cell lines were misclassified. Specific mutations, such as R175H, R273H, R273L or R273P, which are reported in the literature to exert a DNE, showed the lowest percentage of single heterozygous mutations in vitro (about 5%).We suggest that the currently reported percentage of TP53 single heterozygous mutations in tumour samples and cancer cell lines is overestimated. Thus, the magnitude of the DNE of TP53 mutations is questionable. This scepticism is supported by database investigations showing that retention of the wild-type allele occurs with the same frequency as either nonsense or missense TP53 mutations.Single heterozygous mutations of TP53 are associated with gain-of-function (GOF) phenomena and, especially, the dominant-negative effect (DNE) [1,2]. Nonetheless, GOF can be attributed to hemizygous or homozygous, as well as heterozygous, mutations [3]. DNE may be linked to many processes, including the effectiveness of chemotherapy and the failure of TP53 gene therapy [4,5]. Dominant-negative TP53 mutations are frequ

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