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载脂蛋白B编辑酶催化多肽样蛋白3(APOBEC3)区域的种系变异与癌症风险的关联以及肿瘤中APOBEC特征性突变的富集

Association of germline variants in the APOBEC3 region with cancer risk and enrichment with APOBEC-signature mutations in tumors.

作者信息

Middlebrooks Candace D, Banday A Rouf, Matsuda Konichi, Udquim Krizia-Ivana, Onabajo Olusegun O, Paquin Ashley, Figueroa Jonine D, Zhu Bin, Koutros Stella, Kubo Michiaki, Shuin Taro, Freedman Neal D, Kogevinas Manolis, Malats Nuria, Chanock Stephen J, Garcia-Closas Montserrat, Silverman Debra T, Rothman Nathaniel, Prokunina-Olsson Ludmila

机构信息

Laboratory of Translational Genomics, Division of Cancer Epidemiology and Genetics, National Cancer Institute, US National Institutes of Health, Bethesda, Maryland, USA.

Laboratory of Molecular Medicine, Human Genome Center, Institute of Medical Science, University of Tokyo, Tokyo, Japan.

出版信息

Nat Genet. 2016 Nov;48(11):1330-1338. doi: 10.1038/ng.3670. Epub 2016 Sep 19.

DOI:10.1038/ng.3670
PMID:27643540
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6583788/
Abstract

High rates of APOBEC-signature mutations are found in many tumors, but factors affecting this mutation pattern are not well understood. Here we explored the contribution of two common germline variants in the APOBEC3 region. SNP rs1014971 was associated with bladder cancer risk, increased APOBEC3B expression, and enrichment with APOBEC-signature mutations in bladder tumors. In contrast, a 30-kb deletion that eliminates APOBEC3B and creates an APOBEC3A-APOBEC3B chimera was not important in bladder cancer, whereas it was associated with breast cancer risk and enrichment with APOBEC-signature mutations in breast tumors. In vitro, APOBEC3B expression was predominantly induced by treatment with a DNA-damaging drug in bladder cancer cell lines, and APOBEC3A expression was induced as part of the antiviral interferon-stimulated response in breast cancer cell lines. These findings suggest a tissue-specific role of environmental oncogenic triggers, particularly in individuals with germline APOBEC3 risk variants.

摘要

在许多肿瘤中都发现了高频率的载脂蛋白B编辑复合体(APOBEC)特征性突变,但影响这种突变模式的因素尚未完全明确。在此,我们探究了APOBEC3区域中两种常见种系变体的作用。单核苷酸多态性(SNP)rs1014971与膀胱癌风险、APOBEC3B表达增加以及膀胱肿瘤中APOBEC特征性突变的富集有关。相比之下,一个30千碱基的缺失消除了APOBEC3B并产生了一个APOBEC3A-APOBEC3B嵌合体,在膀胱癌中并不重要,而它与乳腺癌风险以及乳腺肿瘤中APOBEC特征性突变的富集有关。在体外,APOBEC3B的表达主要是由膀胱癌细胞系中DNA损伤药物处理诱导的,而APOBEC3A的表达是作为乳腺癌细胞系中抗病毒干扰素刺激反应的一部分被诱导的。这些发现表明环境致癌触发因素具有组织特异性作用,尤其是在携带种系APOBEC3风险变体的个体中。

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Mutation Processes in 293-Based Clones Overexpressing the DNA Cytosine Deaminase APOBEC3B.过表达DNA胞嘧啶脱氨酶APOBEC3B的293细胞系克隆中的突变过程
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An APOBEC3A hypermutation signature is distinguishable from the signature of background mutagenesis by APOBEC3B in human cancers.在人类癌症中,载脂蛋白B mRNA编辑酶催化多肽样3A(APOBEC3A)超突变特征可与载脂蛋白B mRNA编辑酶催化多肽样3B(APOBEC3B)引起的背景诱变特征区分开来。
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