Blood Leukocyte DNA Methylation Markers of Periodontal Disease and Risk of Lung Cancer in a Case-Control Study Nested in the CLUE II Cohort.

IF 3.7 3区 医学 Q2 ONCOLOGY Cancer Epidemiology Biomarkers & Prevention Pub Date : 2024-10-02 DOI:10.1158/1055-9965.EPI-24-0279
Rachel Mulvaney, Yongyi Pan, Naisi Zhao, Flavia Teles, Jiayun Lu, Elizabeth A Platz, Karl T Kelsey, Dominique S Michaud
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Abstract

Background: Periodontal disease and DNA methylation markers have separately been associated with lung cancer risk. Examining methylation levels at genomic regions previously linked to periodontal disease may provide insights on the link between periodontal disease and lung cancer.

Methods: In a nested case-control study drawn from the CLUE II cohort, we measured DNA methylation levels in 208 lung cancer cases and 208 controls. We examined the association between 37 DNA-methylated 5'-C-phosphate-G-3' (CpG) sites at three genomic regions, homeobox 4 (HOXA4), zinc finger protein (ZFP57), and a long noncoding RNA gene located in Chr10 (ENSG00000231601), and lung cancer risk.

Results: Statistically significant associations with lung cancer risk were observed for all 14 CpG sites from HOXA4 (OR ranging 1.41-1.62 for 1 SD increase in the DNA methylation level, especially within 15 years) and 1 CpG site on gene ENSG00000231601 (OR = 1.34 for 1 SD increase in the DNA methylation level). Although CpG sites on gene ZFP57 were not associated with lung cancer risk overall, statistically significant inverse associations were noted for six CpG sites when restricting follow-up to 15 years (OR = 0.73-0.77 for 1 SD increase in the DNA methylation level).

Conclusions: Key methylation levels associated with periodontal disease are also associated with lung cancer risk. For both HOXA4 and ZFP57, the associations were stronger within 15 years of follow-up, which suggest that, if causal, the impact of methylation is acting late in the natural history of lung cancer.

Impact: Identifying biological pathways that link periodontal disease and lung cancer could provide new opportunities for lung cancer detection and prevention.

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嵌套于 CLUE II 队列的一项病例对照研究中牙周病和肺癌风险的血白细胞 DNA 甲基化标记。
背景:牙周病和DNA甲基化标记分别与肺癌风险有关。研究以前与牙周病相关的基因组区域的甲基化水平,可能有助于深入了解牙周病与肺癌之间的联系:在一项来自 CLUE II 队列的嵌套病例对照研究中,我们测量了 208 例肺癌病例和 208 例对照组的 DNA 甲基化水平。我们检测了三个基因组区域(Homeobox 4 (HOXA4)、锌指蛋白 (ZFP57) 和位于 Chr10 (ENSG00000231601)的 lcRNA 基因区域)的 37 个 DNA 甲基化 CpG 位点与肺癌风险之间的关联:HOXA4的所有14个CpG位点(甲基化水平每增加1 SD,几率比[OR]为1.41-1.62,尤其是在15年内)和基因ENSG00000231601的一个CpG位点(DNA甲基化水平每增加1 SD,几率比=1.34)都与肺癌风险有统计学意义。虽然基因 ZFP57 上的 CpG 位点总体上与肺癌风险无关,但如果将随访时间限制在 15 年,则有 6 个 CpGs 存在统计学意义上的显著反向关联(甲基化水平每增加 1 SD,OR=0.73-0.77):结论:与牙周病相关的关键甲基化变化也与肺癌风险有关。结论:与牙周病相关的关键甲基化变化也与肺癌风险有关。对于HOXA4和ZFP57,这些关联在15年的随访中更为强烈,这表明它们在肺癌自然史中起作用的时间较晚:影响:确定将牙周病与肺癌联系起来的生物学途径可为肺癌的检测和预防提供新的机会。
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来源期刊
Cancer Epidemiology Biomarkers & Prevention
Cancer Epidemiology Biomarkers & Prevention 医学-公共卫生、环境卫生与职业卫生
CiteScore
6.50
自引率
2.60%
发文量
538
审稿时长
1.6 months
期刊介绍: Cancer Epidemiology, Biomarkers & Prevention publishes original peer-reviewed, population-based research on cancer etiology, prevention, surveillance, and survivorship. The following topics are of special interest: descriptive, analytical, and molecular epidemiology; biomarkers including assay development, validation, and application; chemoprevention and other types of prevention research in the context of descriptive and observational studies; the role of behavioral factors in cancer etiology and prevention; survivorship studies; risk factors; implementation science and cancer care delivery; and the science of cancer health disparities. Besides welcoming manuscripts that address individual subjects in any of the relevant disciplines, CEBP editors encourage the submission of manuscripts with a transdisciplinary approach.
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