DNA损伤修复基因启动子中非小细胞肺癌致病变异的系统鉴定
Systematic identification of pathogenic variants of non-small cell lung cancer in the promoters of DNA-damage repair genes.
作者信息
An Mingxing, Chen Congcong, Xiang Jun, Li Yang, Qiu Pinyu, Tang Yiru, Liu Xinyue, Gu Yayun, Qin Na, He Yuanlin, Zhu Meng, Jiang Yue, Dai Juncheng, Jin Guangfu, Ma Hongxia, Wang Cheng, Hu Zhibin, Shen Hongbing
机构信息
Department of Epidemiology, School of Public Health, Southeast University, Nanjing, Jiangsu, China; Department of Epidemiology, Center for Global Health, School of Public Health, Nanjing Medical University, Nanjing, Jiangsu 211166, China.
Department of Epidemiology, Center for Global Health, School of Public Health, Nanjing Medical University, Nanjing, Jiangsu 211166, China; The Second People's Hospital of Changzhou, The Third Affiliated Hospital of Nanjing Medical University, Changzhou Medical Center, Nanjing Medical University, Changzhou 213003, China.
出版信息
EBioMedicine. 2024 Dec;110:105480. doi: 10.1016/j.ebiom.2024.105480. Epub 2024 Dec 3.
BACKGROUND
Deficiency in DNA-damage repair (DDR) genes, often due to disruptive coding variants, is linked to higher cancer risk. Our previous study has revealed the association between rare loss-of-function variants in DDR genes and the risk of lung cancer. However, it is still challenging to study the predisposing role of rare regulatory variants of these genes.
METHODS
Based on whole-genome sequencing data from 2984 patients with non-small cell lung cancer (NSCLC) and 3020 controls, we performed massively parallel reporter assays on 1818 rare variants located in the promoters of DDR genes. Pathway- or gene-level burden analyses were performed using Firth's logistic regression or generalized linear model.
FINDINGS
We identified 750 rare functional regulatory variants (frVars) that showed allelic differences in transcriptional activity within the promoter regions of DDR genes. Interestingly, the burden of frVars was significantly elevated in cases (odds ratio [OR] = 1.17, p = 0.026), whereas the burden of variants prioritized solely based on bioinformatics annotation was comparable between cases and controls (OR = 1.04, p = 0.549). Among the frVars, 297 were down-regulated transcriptional activity (dr-frVars) and 453 were up-regulated transcriptional activity (ur-frVars); especially, dr-frVars (OR = 1.30, p = 0.008) rather than ur-frVars (OR = 1.06, p = 0.495) were significantly associated with risk of NSCLC. Individuals with NSCLC carried more dr-frVars from Fanconi anemia, homologous recombination, and nucleotide excision repair pathways. In addition, we identified seven genes (i.e., BRCA2, GTF2H1, DDB2, BLM, ALKBH2, APEX1, and RAD51B) with promoter dr-frVars that were associated with lung cancer susceptibility.
INTERPRETATION
Our findings indicate that functional promoter variants in DDR genes, in addition to protein-truncating variants, can be pathogenic and contribute to lung cancer susceptibility.
FUNDING
National Natural Science Foundation of China, Youth Foundation of Jiangsu Province, Research Unit of Prospective Cohort of Cardiovascular Diseases and Cancer of Chinese Academy of Medical Sciences, and Natural Science Foundation of Jiangsu Province.
背景
DNA损伤修复(DDR)基因缺陷通常由破坏性编码变异引起,与较高的癌症风险相关。我们之前的研究揭示了DDR基因中罕见的功能丧失变异与肺癌风险之间的关联。然而,研究这些基因罕见调控变异的易感性作用仍然具有挑战性。
方法
基于2984例非小细胞肺癌(NSCLC)患者和3020例对照的全基因组测序数据,我们对位于DDR基因启动子区域的1818个罕见变异进行了大规模平行报告基因检测。使用Firth逻辑回归或广义线性模型进行通路或基因水平的负担分析。
结果
我们鉴定出750个罕见的功能调控变异(frVars),这些变异在DDR基因启动子区域的转录活性上表现出等位基因差异。有趣的是,病例组中frVars的负担显著升高(优势比[OR]=1.17,p=0.026),而仅基于生物信息学注释优先选择的变异在病例组和对照组之间的负担相当(OR=1.04,p=0.549)。在frVars中,297个是转录活性下调的变异(dr-frVars),453个是转录活性上调的变异(ur-frVars);特别是,dr-frVars(OR=1.30,p=0.008)而非ur-frVars(OR=1.06,p=0.495)与NSCLC风险显著相关。NSCLC患者携带更多来自范可尼贫血、同源重组和核苷酸切除修复通路的dr-frVars。此外,我们鉴定出7个具有启动子dr-frVars且与肺癌易感性相关的基因(即BRCA2、GTF2H1、DDB2、BLM、ALKBH2、APEX1和RAD51B)。
解读
我们的研究结果表明,DDR基因中的功能性启动子变异除了蛋白质截短变异外,也可能具有致病性并导致肺癌易感性。
资助
中国国家自然科学基金、江苏省青年基金、中国医学科学院心血管疾病和癌症前瞻性队列研究室、江苏省自然科学基金。
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