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利用 Cg05575921 甲基化预测肺癌风险:一种潜在无偏的精准表观遗传学方法。

Using Cg05575921 methylation to predict lung cancer risk: a potentially bias-free precision epigenetics approach.

机构信息

Behavioural Diagnostics LLC, Coralville, IA, USA.

Department of Psychiatry, University of Iowa, Iowa City, IA, USA.

出版信息

Epigenetics. 2022 Dec;17(13):2096-2108. doi: 10.1080/15592294.2022.2108082. Epub 2022 Aug 3.

DOI:10.1080/15592294.2022.2108082
PMID:35920547
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9665144/
Abstract

The decision to engage in lung cancer screening (LCS) necessitates weighing benefits versus harms. Previously, clinicians in the United States have used the PLCOM algorithm to guide LCS decision-making. However, that formula contains race and gender-based variables. Previously, using data from a European study, Bojesen and colleagues have suggested that cg05575921 methylation could guide decision-making. To test this hypothesis in a more diverse American population, we examined DNA and clinical data from 3081 subjects from the National Lung Screening Trial (NLST) study. Using survival analysis, we found a simple linear predictor consisting of age, pack-year consumption and cg05575921, to have the best predictive power among several alternatives (AUC = 0.66). Results showed that the highest quartile of risk was more than 2-fold more likely to develop lung cancer than those in the lowest quartile. Race, ethnicity, and gender had no effect on prediction with both cg05575921 and pack years contributing equally (both p < 0.003) to risk prediction. Current smokers had considerably lower methylation than former smokers (46% vs 67%; p < 0.001) with the average methylation of those who quit approaching 80% after 25 years of cessation. Finally, current male smokers had lower mean cg05575921 percentage than female smokers (46% vs 49%; p < 0.001). We conclude that cg05575921 (along with age and pack years) can be used to guide LCS decision-making, and additional studies might focus on how best to use methylation to inform decision-making.

摘要

参与肺癌筛查(LCS)需要权衡利弊。 以前,美国的临床医生使用 PLCOM 算法来指导 LCS 决策。 但是,该公式包含基于种族和性别的变量。 以前,使用来自欧洲研究的数据,Bojesen 及其同事提出 cg05575921 甲基化可以指导决策。 为了在更多样化的美国人群中检验这一假设,我们检查了来自国家肺癌筛查试验(NLST)研究的 3081 名受试者的 DNA 和临床数据。 使用生存分析,我们发现由年龄,吸烟包年数和 cg05575921 组成的简单线性预测因子在几种替代方案中具有最佳的预测能力(AUC=0.66)。 结果表明,最高四分位的风险是最低四分位的两倍以上,更有可能发展为肺癌。 种族,民族和性别对 cg05575921 和吸烟包年数的预测均无影响(两者均 p<0.003),均对风险预测有贡献。 当前吸烟者的甲基化水平明显低于前吸烟者(46%比 67%;p<0.001),戒烟 25 年后,平均甲基化水平接近 80%。 最后,当前男性吸烟者的 cg05575921 百分比均值低于女性吸烟者(46%比 49%;p<0.001)。 我们得出结论,cg05575921(与年龄和吸烟包年数)可用于指导 LCS 决策,并且其他研究可能侧重于如何最好地使用甲基化来为决策提供信息。

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