Germline variants of homology-directed repair or mismatch repair genes in cervical cancer.

IF 5.7 2区 医学 Q1 ONCOLOGY International Journal of Cancer Pub Date : 2024-10-23 DOI:10.1002/ijc.35221
Lara Kokemüller, Dhanya Ramachandran, Peter Schürmann, Robert Geffers, Matthias Jentschke, Gerd Böhmer, Hans-Georg Strauß, Christine Hirchenhain, Monika Schmidmayr, Florian Müller, Peter A Fasching, Alexander Luyten, Norman Häfner, Peter Hillemanns, Thilo Dörk
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Abstract

While cervical cancer is associated with a persistent human papillomavirus (HPV) infection, the progression to cancer is influenced by genomic risk factors that have remained largely obscure. Pathogenic variants in genes of the homology-directed repair (HDR) or mismatch repair (MMR) are known to predispose to diverse tumour entities including breast and ovarian cancer (HDR) or colon and endometrial cancer (MMR). We here investigate the spectrum of HDR and MMR germline variants in cervical cancer, with particular focus on the HPV status and histological subgroups. We performed targeted next-generation sequencing for 5 MMR genes and 12 HDR genes on 728 German patients with cervical dysplasia or invasive cancer. In total, 4% of our patients carried a pathogenic germline variant, based on ClinVar classifications and additional ESM1b and AlphaMissense predictions. These included 15 patients with truncating variants in HDR genes (BARD1, BRCA1, BRCA2, BRIP1, FANCM, RAD51D and SLX4). MMR-related gene variants were less prevalent and mainly of the missense type. While MMR-related gene variants tended to associate with adenocarcinomas, HDR gene variants were commonly observed in squamous cancers. While one patient with HPV-negative cancer carried a pathogenic MMR gene variant (in MSH6), the HDR germline variants were found in patients with HPV-positive cancers and tended to associate with HPV18. Taken together, our study supports a potentially risk-modifying role of MMR and HDR germline variants in cervical cancer but no association with HPV-negative status. These variants may be exploitable in future therapeutic managements.

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宫颈癌中同源定向修复或错配修复基因的种系变异。
虽然宫颈癌与人类乳头瘤病毒(HPV)的持续感染有关,但癌症的进展受基因组风险因素的影响,而这些因素在很大程度上仍不为人所知。已知同源定向修复(HDR)或错配修复(MMR)基因中的致病变异易导致多种肿瘤,包括乳腺癌和卵巢癌(HDR)或结肠癌和子宫内膜癌(MMR)。我们在此研究了宫颈癌中的 HDR 和 MMR 基因变异谱,尤其关注 HPV 状态和组织学亚群。我们对 728 名德国宫颈发育不良或浸润癌患者的 5 个 MMR 基因和 12 个 HDR 基因进行了有针对性的新一代测序。根据ClinVar分类以及ESM1b和AlphaMissense的额外预测,共有4%的患者携带致病性种系变异。其中15名患者的HDR基因(BARD1、BRCA1、BRCA2、BRIP1、FANCM、RAD51D和SLX4)存在截短变异。与 MMR 相关的基因变异发生率较低,主要为错义类型。MMR 相关基因变异往往与腺癌有关,而 HDR 基因变异则常见于鳞癌。一名HPV阴性癌症患者携带致病性MMR基因变异(MSH6),而HDR种系变异则在HPV阳性癌症患者中发现,且往往与HPV18有关。综上所述,我们的研究支持 MMR 和 HDR 种系变异在宫颈癌中具有潜在的风险调节作用,但与 HPV 阴性状态无关。这些变异可用于未来的治疗管理。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
13.40
自引率
3.10%
发文量
460
审稿时长
2 months
期刊介绍: The International Journal of Cancer (IJC) is the official journal of the Union for International Cancer Control—UICC; it appears twice a month. IJC invites submission of manuscripts under a broad scope of topics relevant to experimental and clinical cancer research and publishes original Research Articles and Short Reports under the following categories: -Cancer Epidemiology- Cancer Genetics and Epigenetics- Infectious Causes of Cancer- Innovative Tools and Methods- Molecular Cancer Biology- Tumor Immunology and Microenvironment- Tumor Markers and Signatures- Cancer Therapy and Prevention
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