升高的载脂蛋白B编辑酶催化多肽样3B（APOBEC3B）表达在p53缺陷细胞中驱动一种类似kataegic的突变特征和与复制应激相关的治疗易感性。

Elevated APOBEC3B expression drives a kataegic-like mutation signature and replication stress-related therapeutic vulnerabilities in p53-defective cells.

作者信息

Nikkilä Jenni, Kumar Rahul, Campbell James, Brandsma Inger, Pemberton Helen N, Wallberg Fredrik, Nagy Kinga, Scheer Ildikó, Vertessy Beata G, Serebrenik Artur A, Monni Valentina, Harris Reuben S, Pettitt Stephen J, Ashworth Alan, Lord Christopher J

机构信息

The CRUK Gene Function Laboratory and The Breast Cancer Now Toby Robins Breast Cancer Research Centre, The Institute of Cancer Research, London SW3 6JB, UK.

FACS Facility, The Institute of Cancer Research, London SW3 6JB, UK.

出版信息

Br J Cancer. 2017 Jun 27;117(1):113-123. doi: 10.1038/bjc.2017.133. Epub 2017 May 23.

DOI:10.1038/bjc.2017.133

PMID:28535155

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5520199/

Abstract

BACKGROUND

Elevated APOBEC3B expression in tumours correlates with a kataegic pattern of localised hypermutation. We assessed the cellular phenotypes associated with high-level APOBEC3B expression and the influence of p53 status on these phenotypes using an isogenic system.

METHODS

We used RNA interference of p53 in cells with inducible APOBEC3B and assessed DNA damage response (DDR) biomarkers. The mutational effects of APOBEC3B were assessed using whole-genome sequencing. In vitro small-molecule inhibitor sensitivity profiling was used to identify candidate therapeutic vulnerabilities.

RESULTS

Although APOBEC3B expression increased the incorporation of genomic uracil, invoked DDR biomarkers and caused cell cycle arrest, inactivation of p53 circumvented APOBEC3B-induced cell cycle arrest without reversing the increase in genomic uracil or DDR biomarkers. The continued expression of APOBEC3B in p53-defective cells not only caused a kataegic mutational signature but also caused hypersensitivity to small-molecule DDR inhibitors (ATR, CHEK1, CHEK2, PARP, WEE1 inhibitors) as well as cisplatin/ATR inhibitor and ATR/PARP inhibitor combinations.

CONCLUSIONS

Although loss of p53 might allow tumour cells to tolerate elevated APOBEC3B expression, continued expression of this enzyme might impart a number of therapeutic vulnerabilities upon tumour cells.

摘要

背景

肿瘤中载脂蛋白B mRNA编辑酶催化多肽样3B（APOBEC3B）表达升高与局部超突变的剧烈模式相关。我们使用同基因系统评估了与高水平APOBEC3B表达相关的细胞表型以及p53状态对这些表型的影响。

方法

我们在可诱导APOBEC3B的细胞中对p53进行RNA干扰，并评估DNA损伤反应（DDR）生物标志物。使用全基因组测序评估APOBEC3B的突变效应。体外小分子抑制剂敏感性分析用于确定候选治疗靶点。

结果

尽管APOBEC3B表达增加了基因组尿嘧啶的掺入，引发了DDR生物标志物并导致细胞周期停滞，但p53失活规避了APOBEC3B诱导的细胞周期停滞，而没有逆转基因组尿嘧啶或DDR生物标志物的增加。在p53缺陷细胞中持续表达APOBEC3B不仅导致剧烈的突变特征，还导致对小分子DDR抑制剂（ATR、CHEK1、CHEK2、PARP、WEE1抑制剂）以及顺铂/ATR抑制剂和ATR/PARP抑制剂组合的超敏反应。

结论

虽然p53缺失可能使肿瘤细胞耐受升高的APOBEC3B表达，但这种酶的持续表达可能会使肿瘤细胞产生许多治疗靶点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4346/5520199/5e5e2e1cb92c/bjc2017133f1.jpg

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升高的载脂蛋白B编辑酶催化多肽样3B（APOBEC3B）表达在p53缺陷细胞中驱动一种类似kataegic的突变特征和与复制应激相关的治疗易感性。

Elevated APOBEC3B expression drives a kataegic-like mutation signature and replication stress-related therapeutic vulnerabilities in p53-defective cells.

作者信息

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出版信息

BACKGROUND

METHODS

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方法

结果

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