Abstract

BackgroundRecently published data showed discrepancies beteween P53 cDNA and DNA sequencing in glioblastomas. We hypothesised that similar discrepancies may be observed in other human cancers.MethodsTo this end, we analyzed 23 colorectal cancers for P53 mutations and gene expression using both DNA and cDNA sequencing, real-time PCR and immunohistochemistry.ResultsWe found P53 gene mutations in 16 cases (15 missense and 1 nonsense). Two of the 15 cases with missense mutations showed alterations based only on cDNA, and not DNA sequencing. Moreover, in 6 of the 15 cases with a cDNA mutation those mutations were difficult to detect in the DNA sequencing, so the results of DNA analysis alone could be misinterpreted if the cDNA sequencing results had not also been available. In all those 15 cases, we observed a higher ratio of the mutated to the wild type template by cDNA analysis, but not by the DNA analysis. Interestingly, a similar overexpression of P53 mRNA was present in samples with and without P53 mutations.ConclusionIn terms of colorectal cancer, those discrepancies might be explained under three conditions: 1, overexpression of mutated P53 mRNA in cancer cells as compared with normal cells; 2, a higher content of cells without P53 mutation (normal cells and cells showing K-RAS and/or APC but not P53 mutation) in samples presenting P53 mutation; 3, heterozygous or hemizygous mutations of P53 gene. Additionally, for heterozygous mutations unknown mechanism(s) causing selective overproduction of mutated allele should also be considered. Our data offer new clues for studying discrepancy in P53 cDNA and DNA sequencing analysis.

Highlights

  • Published data showed discrepancies beteween P53 cDNA and DNA sequencing in glioblastomas

  • In a recently published study, we showed the prevalence of the mutated P53 template by cDNA sequencing and determination of the wild type template by DNA analysis in glioblastomas (GBM)

  • DNA sequencing performed for 15 samples with missense mutation detected P53 gene mutation only in six samples, in another six cases, the mutated template was difficult to detect, in the final two cases the DNA analyses did not revealed a P53 gene alteration

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Summary

Introduction

Published data showed discrepancies beteween P53 cDNA and DNA sequencing in glioblastomas. We hypothesised that similar discrepancies may be observed in other human cancers. In a recently published study, we showed the prevalence of the mutated P53 template by cDNA sequencing and determination of the wild type template by DNA analysis in glioblastomas (GBM). We decided to test if similar discrepancies occur in other human cancers. The P53 gene status was evaluated by means of both cDNA and DNA sequencing, real-time RT-PCR and immunohistochemistry. This comprehensive approach allowed us to go toward an explanation of divergent results observed following cDNA and DNA P53 sequencing. Our investigation sheds new light on the discrepancies between immunohistochemical and molecular analyses of P53 in CC

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