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乳腺癌中密码子 72 多态性与 p53 体细胞突变的联合生存效应取决于种族和分子亚型。

The combined survival effect of codon 72 polymorphisms and p53 somatic mutations in breast cancer depends on race and molecular subtype.

机构信息

Department of Pathology, University of Alabama at Birmingham, Birmingham, AL, United States of America.

出版信息

PLoS One. 2019 Feb 7;14(2):e0211734. doi: 10.1371/journal.pone.0211734. eCollection 2019.

Abstract

BACKGROUND

The codon 72 polymorphism in the p53 gene relates to the risk of breast cancer (BC), but this relationship in racially diverse populations is not known. The present study examined the prognostic value of this polymorphism for African American (AA) and Caucasian (CA) BC patients separately and considered the confounding variables of molecular subtypes and somatic mutations in p53.

METHODS

Tissue sections of BCs from 116 AAs and 160 CAs were evaluated for p53 mutations and genotyped for the codon 72 polymorphism. The relationships of phenotypes to clinicopathologic features were determined by χ2 analyses; patient survival was estimated by Kaplan-Meier univariate and Cox regression multivariate models in a retrospective cohort study design.

RESULTS

The proportion of single nucleotide polymorphism (SNP) 72 alleles differed for races. Many cancers of AAs were Pro/Pro, but most for CAs were Arg/Arg. A higher frequency of missense p53 mutations was evident for AAs. There was an interaction between the SNP allele and p53 mutations for AA women only. The proportion of women with both the Pro/Pro allele and a p53 somatic mutation was higher for AA than CA women. The interaction between missense p53 mutations and Pro/Pro had a negative effect on survival, particularly for AAs with luminal cancers.

CONCLUSIONS

For BCs, the survival effect of SNP72 combined with a p53 missense mutation is dependent on race and molecular subtype. Although such a mutation is a marker of poor prognosis, it is relevant to identify the variant Pro/Pro in the case of AAs, especially those with luminal subtypes of BC.

摘要

背景

p53 基因的密码子 72 多态性与乳腺癌(BC)的风险相关,但在不同种族的人群中,这种关系尚不清楚。本研究分别检查了该多态性对非裔美国人和高加索裔 BC 患者的预后价值,并考虑了分子亚型和 p53 体细胞突变的混杂变量。

方法

对 116 名非裔美国人和 160 名高加索裔的 BC 组织切片进行 p53 突变检测,并对密码子 72 多态性进行基因分型。通过 χ2 分析确定表型与临床病理特征的关系;在回顾性队列研究设计中,通过 Kaplan-Meier 单变量和 Cox 回归多变量模型估计患者的生存情况。

结果

种族之间 SNP72 等位基因的比例不同。许多非裔美国人的癌症是 Pro/Pro,但大多数高加索裔的癌症是 Arg/Arg。非裔美国人的错义 p53 突变频率更高。只有非裔美国女性的 SNP 等位基因和 p53 突变之间存在相互作用。同时具有 Pro/Pro 等位基因和 p53 体细胞突变的女性比例在非裔美国女性中高于高加索裔女性。错义 p53 突变和 Pro/Pro 的相互作用对生存有负面影响,特别是对具有腔型癌症的非裔美国人。

结论

对于 BC,SNP72 与 p53 错义突变的联合生存效应取决于种族和分子亚型。尽管这种突变是预后不良的标志,但对于非裔美国人,特别是具有腔型 BC 的患者,识别变体 Pro/Pro 是相关的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e193/6366783/e3ceef9a1157/pone.0211734.g001.jpg

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