与子宫颈癌中突变特征、DNA损伤修复及染色质重塑途径相关的基因组改变

Genomic alterations associated with mutational signatures, DNA damage repair and chromatin remodeling pathways in cervical carcinoma.

作者信息

Halle Mari K, Sundaresan Aishwarya, Zhang Jianqing, Pedamallu Chandra Sekhar, Srinivasasainagendra Vinodh, Blair Jessica, Brooke Dewey, Bertelsen Bjørn I, Woie Kathrine, Shrestha Sadeep, Tiwari Hemant, Wong Yick Fu, Krakstad Camilla, Ojesina Akinyemi I

机构信息

Department of Obstetrics and Gynaecology, Haukeland University Hospital, Bergen, Norway.

Centre for Cancer Biomarkers, Department of Clinical Science, University of Bergen, Bergen, Norway.

出版信息

NPJ Genom Med. 2021 Oct 7;6(1):82. doi: 10.1038/s41525-021-00244-2.

DOI:10.1038/s41525-021-00244-2

PMID:34620846

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8497615/

Abstract

Despite recent advances in the prevention of cervical cancer, the disease remains a leading cause of cancer-related deaths in women worldwide. By applying the GISTIC2.0 and/or the MutSig2CV algorithms on 430 whole-exome-sequenced cervical carcinomas, we identified previously unreported significantly mutated genes (SMGs) (including MSN, GPX1, SPRED3, FAS, and KRT8), amplifications (including NFIA, GNL1, TGIF1, and WDR87) and deletions (including MIR562, PVRL1, and NTM). Subset analyses of 327 squamous cell carcinomas and 86 non-squamous cell carcinomas revealed previously unreported SMGs in BAP1 and IL28A, respectively. Distinctive copy number alterations related to tumors predominantly enriched for CpG- and TpC mutations were observed. CD274, GRB2, KRAS, and EGFR were uniquely significantly amplified within the Tp*C-enriched tumors. A high frequency of aberrations within DNA damage repair and chromatin remodeling genes were detected. Facilitated by the large sample size derived from combining multiple datasets, this study reveals potential targets and prognostic markers for cervical cancer.

摘要

尽管近年来在宫颈癌预防方面取得了进展，但该疾病仍是全球女性癌症相关死亡的主要原因。通过对430例全外显子测序的宫颈癌应用GISTIC2.0和/或MutSig2CV算法，我们鉴定出了先前未报道的显著突变基因（SMG）（包括MSN、GPX1、SPRED3、FAS和KRT8）、扩增（包括NFIA、GNL1、TGIF1和WDR87）以及缺失（包括MIR562、PVRL1和NTM）。对327例鳞状细胞癌和86例非鳞状细胞癌的亚组分析分别揭示了BAP1和IL28A中先前未报道的SMG。观察到与主要富含CpG和TpC突变的肿瘤相关的独特拷贝数改变。CD274、GRB2、KRAS和EGFR在富含TpC的肿瘤中独特地显著扩增。检测到DNA损伤修复和染色质重塑基因中的高频畸变。本研究借助合并多个数据集获得的大样本量，揭示了宫颈癌的潜在靶点和预后标志物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/41fe/8497615/08c39a60bbc1/41525_2021_244_Fig1_HTML.jpg

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与子宫颈癌中突变特征、DNA损伤修复及染色质重塑途径相关的基因组改变

Genomic alterations associated with mutational signatures, DNA damage repair and chromatin remodeling pathways in cervical carcinoma.

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