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P53 mutant breast cancer patients expressing p53? have as good a prognosis as wild-type p53 breast cancer patients.


ABSTRACT:

Introduction

Normal function of the p53 network is lost in most cancers, often through p53 mutation. The clinical impact of p53 mutations in breast cancer remains uncertain, especially where p53 isoforms may modify the effects of these p53 mutations.

Methods

Expression of p53? and p53? isoforms, the isoforms identified in normal breast tissue, was detected by reverse transcription polymerase chain reaction from a cohort of 127 primary breast tumours. Expression of p53? and p53? isoforms was analysed in relation to clinical markers and clinical outcomes (5 years) by binary logistic regression, Cox proportional hazards regression and Kaplan-Meier survival analyses.

Results

p53? and p53? were not randomly expressed in breast cancer. p53? was associated with tumour oestrogen receptor (ER) expression, and p53? was associated with mutation of the p53 gene. The patient group with the mutant p53 breast tumour-expressing p53? isoform had low cancer recurrence and an overall survival as good as that of patients with wild-type p53 breast cancer. Conversely, patients expressing only mutant p53, without p53? isoform expression, had a particularly poor prognosis.

Conclusions

The determination of p53? expression may allow the identification, independently of the ER status, of two subpopulations of mutant p53 breast cancer patients, one expressing p53? with a prognosis as good as the wild-type p53 breast cancer patients and a second one not expressing p53? with a particularly poor prognosis. The p53? isoform may provide an explanation of the hitherto inconsistent relationship between p53 mutation, treatment response and outcome in breast cancer.

SUBMITTER: Bourdon JC 

PROVIDER: S-EPMC3109573 | biostudies-literature | 2011 Jan

REPOSITORIES: biostudies-literature

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Publications

p53 mutant breast cancer patients expressing p53γ have as good a prognosis as wild-type p53 breast cancer patients.

Bourdon Jean-Christophe JC   Khoury Marie P MP   Diot Alexandra A   Baker Lee L   Fernandes Kenneth K   Aoubala Mustapha M   Quinlan Philip P   Purdie Colin A CA   Jordan Lee B LB   Prats Anne-Catherine AC   Lane David P DP   Thompson Alastair M AM  

Breast cancer research : BCR 20110120 1


<h4>Introduction</h4>Normal function of the p53 network is lost in most cancers, often through p53 mutation. The clinical impact of p53 mutations in breast cancer remains uncertain, especially where p53 isoforms may modify the effects of these p53 mutations.<h4>Methods</h4>Expression of p53β and p53γ isoforms, the isoforms identified in normal breast tissue, was detected by reverse transcription polymerase chain reaction from a cohort of 127 primary breast tumours. Expression of p53β and p53γ is  ...[more]

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