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乳腺癌中与TP53异常相关的基因组不稳定和预后不良。分子和免疫组织化学分析。

Genomic instability and poor prognosis associated with abnormal TP53 in breast carcinomas. Molecular and immunohistochemical analysis.

作者信息

Valgardsdottir R, Tryggvadottir L, Steinarsdottir M, Olafsdottir K, Jonasdottir S, Jonasson J G, Ogmundsdottir H M, Eyfjörd J E

机构信息

Molecular and Cell Biology Research Laboratory, Icelandic Cancer Society, Reykjavik, Iceland.

出版信息

APMIS. 1997 Feb;105(2):121-30. doi: 10.1111/j.1699-0463.1997.tb00550.x.

DOI:10.1111/j.1699-0463.1997.tb00550.x
PMID:9113074
Abstract

Alterations of the TP53 gene were analyzed in samples from 87 primary breast cancer patients, using molecular and immunohistochemical approaches. Mutations were detected in 17% of the samples, using polymerase chain reaction (PCR) and constant denaturant gel electrophoresis (CDGE) on exons 5-8 of the TP53 gene, and were confirmed by sequencing. Abnormal TP53 protein staining was found in 55% of the primary samples, using the monoclonal TP53 antibody DO7. A statistically significant association was found between TP53 mutations and abnormal protein staining (p = 0.002). Our results suggest that dysfunction of the TP53 protein is associated with tumor progression, as we found an association between TP53 abnormalities and accumulation of genetic lesions, measured as overall allelic imbalance (AI), homogeneously staining regions (HSR) and strong ERBB2 overexpression. Furthermore, patients with TP53 mutation had a highly elevated risk of dying from breast cancer during the study period (p < 0.001, RR = 10.68) at a median follow-up time of 42 months. Abnormal TP53 staining was much more frequent than the mutations, but it was not of prognostic significance, whereas strong staining was an independent prognostic factor. We therefore conclude that loss of functional TP53 leads to genetic instability, resulting in poorer short-term prognosis, and that only strong staining of TP53, and not abnormal protein staining in general, is of prognostic significance.

摘要

采用分子和免疫组化方法,对87例原发性乳腺癌患者的样本进行了TP53基因改变分析。利用聚合酶链反应(PCR)和恒变性凝胶电泳(CDGE)对TP53基因的第5 - 8外显子进行检测,在17%的样本中检测到突变,并通过测序得以证实。使用单克隆TP53抗体DO7,在55%的原发性样本中发现了异常的TP53蛋白染色。TP53突变与异常蛋白染色之间存在统计学显著关联(p = 0.002)。我们的结果表明,TP53蛋白功能障碍与肿瘤进展相关,因为我们发现TP53异常与遗传损伤积累之间存在关联,遗传损伤通过总体等位基因失衡(AI)、均匀染色区(HSR)和强烈的ERBB2过表达来衡量。此外,在中位随访时间42个月的研究期间,TP53突变患者死于乳腺癌的风险显著升高(p < 0.001,RR = 10.68)。异常的TP53染色比突变更为常见,但它没有预后意义,而强染色是一个独立的预后因素。因此,我们得出结论,功能性TP53的缺失导致基因不稳定,从而导致较差的短期预后,并且只有TP53的强染色,而不是一般的异常蛋白染色,具有预后意义。

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