非小细胞肺癌 KRAS 基因突变和等位基因特异性亚型的发生率受遗传血统而非自我报告的种族/人种的额外影响。

IF 3.3 Q2 GENETICS & HEREDITY HGG Advances Pub Date : 2024-07-18 Epub Date: 2024-06-19 DOI:10.1016/j.xhgg.2024.100320
Xinan Wang, Kangcheng Hou, Biagio Ricciuti, Joao V Alessi, Xihao Li, Federica Pecci, Rounak Dey, Jia Luo, Mark M Awad, Alexander Gusev, Xihong Lin, Bruce E Johnson, David C Christiani
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引用次数: 0

摘要

KRAS 基因突变是非小细胞肺癌(NSCLC)患者最常见的致癌因素。然而,人们对自我报告的种族和/或民族(SIRE)、基因推断的祖先(GIA)以及它们之间的相互作用如何影响 KRAS 突变还知之甚少。在此,我们研究了波士顿肺癌生存队列和中国 OrigiMed 队列中 3918 名多种族患者的 SIRE、定量 GIA 与 KRAS 突变及其等位基因特异性亚型之间的关系,以及 1450 名 NSCLC 患者的独立验证队列。这项综合分析包括详细的协变量,包括诊断时的年龄、性别、临床分期、癌症组织学和吸烟状况。在调整了潜在的混杂因素后,SIRE-亚洲患者与SIRE-白人患者相比,KRAS突变、反转置换和等位基因特异性亚型KRASG12C的发生率较低。此外,研究还发现,GIA 与 KRAS 基因突变相关,欧洲血统比例较高的患者发生 KRAS 基因突变的风险更高,尤其是发生更多的转换替代和 KRASG12D。值得注意的是,在SIRE-白人患者中,欧洲血统的增加与KRAS突变的可能性增加有关,而美国混血血统的增加与可能性降低有关,这表明定量GIA提供了SIRE之外的额外信息。SIRE、GIA及其与NSCLC中KRAS驱动基因突变的相互作用的关联性突出了将这两者纳入基于人群的癌症研究的重要性,其目的是完善临床决策过程并减少健康差异。
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Additional impact of genetic ancestry over race/ethnicity to prevalence of KRAS mutations and allele-specific subtypes in non-small cell lung cancer.

The KRAS mutation is the most common oncogenic driver in patients with non-small cell lung cancer (NSCLC). However, a detailed understanding of how self-reported race and/or ethnicity (SIRE), genetically inferred ancestry (GIA), and their interaction affect KRAS mutation is largely unknown. Here, we investigated the associations between SIRE, quantitative GIA, and KRAS mutation and its allele-specific subtypes in a multi-ethnic cohort of 3,918 patients from the Boston Lung Cancer Survival cohort and the Chinese OrigiMed cohort with an independent validation cohort of 1,450 patients with NSCLC. This comprehensive analysis included detailed covariates such as age at diagnosis, sex, clinical stage, cancer histology, and smoking status. We report that SIRE is significantly associated with KRAS mutations, modified by sex, with SIRE-Asian patients showing lower rates of KRAS mutation, transversion substitution, and the allele-specific subtype KRASG12C compared to SIRE-White patients after adjusting for potential confounders. Moreover, GIA was found to correlate with KRAS mutations, where patients with a higher proportion of European ancestry had an increased risk of KRAS mutations, especially more transition substitutions and KRASG12D. Notably, among SIRE-White patients, an increase in European ancestry was linked to a higher likelihood of KRAS mutations, whereas an increase in admixed American ancestry was associated with a reduced likelihood, suggesting that quantitative GIA offers additional information beyond SIRE. The association of SIRE, GIA, and their interplay with KRAS driver mutations in NSCLC highlights the importance of incorporating both into population-based cancer research, aiming to refine clinical decision-making processes and mitigate health disparities.

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来源期刊
HGG Advances
HGG Advances Biochemistry, Genetics and Molecular Biology-Molecular Medicine
CiteScore
4.30
自引率
4.50%
发文量
69
审稿时长
14 weeks
期刊最新文献
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