Differences in DNA Methylation-Based Age Prediction Within Twin Pairs Discordant for Cancer.

IF 1 4区 医学 Q4 GENETICS & HEREDITY
Hannes F Bode, Aino Heikkinen, Sara Lundgren, Jaakko Kaprio, Miina Ollikainen
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引用次数: 0

Abstract

DNA methylation-based age acceleration (DNAmAA) is associated with cancer, with both cancer tissue and blood showing increased DNAmAA. We aimed to investigate whether DNAmAA is associated with cancer risk within twin pairs discordant for cancer, and whether DNAmAA has the potential to serve as a biomarker for such. The study included 47 monozygotic and 48 same-sex-dizygotic cancer-discordant twin pairs from the Finnish Twin Cohort study with blood samples available between 17 and 31 years after the cancer diagnosis. We studied all cancers (95 pairs), then separately breast cancer (24 pairs) and all sites other than breast cancer (71 pairs). DNAmAA was calculated for seven models: Horvath, Horvath intrinsic epigenetic age acceleration, Hannum, Hannum intrinsic epigenetic age acceleration, Hannum extrinsic epigenetic age acceleration, PhenoAge and GrimAge. Within-pair differences in DNAmAA were analyzed by paired t tests and linear regression. Twin pairs sampled before cancer diagnosis did not differ significantly in DNAmAA. However, the within-pair differences in DNAmAA before cancer diagnosis increased significantly the closer the cancer diagnosis was, and this acceleration extended for years after the diagnosis. Pairs sampled after the diagnosis differed for DNAmAA with the Horvath models capturing cancer diagnosis-associated DNAmAA across all three cancer groupings. The results suggest that DNAmAA in blood is associated with cancer diagnosis. This may be due to epigenetic alterations in relation to cancer, its treatment or associated lifestyle changes. Based on the current study, the biomarker potential of DNAmAA in blood appears to be limited.

基于DNA甲基化的年龄预测在双胞胎癌症不一致的差异。
基于DNA甲基化的年龄加速(DNAmAA)与癌症有关,癌症组织和血液中都显示出DNAmAA的增加。我们的目的是研究DNAmAA是否与癌症风险不一致的双胞胎中的癌症风险相关,以及DNAmAA是否有潜力作为这种生物标志物。该研究包括来自芬兰双胞胎队列研究的47对同卵双胞胎和48对同性异卵癌症不一致的双胞胎,他们的血液样本在癌症诊断后的17到31年之间。我们研究了所有癌症(95对),然后分别研究了乳腺癌(24对)和除乳腺癌以外的所有部位(71对)。计算Horvath、Horvath内在表观遗传年龄加速、Hannum、Hannum内在表观遗传年龄加速、Hannum外在表观遗传年龄加速、PhenoAge和GrimAge 7种模型的DNAmAA。采用配对t检验和线性回归分析DNAmAA的对内差异。在癌症诊断前取样的双胞胎在DNAmAA上没有显著差异。然而,越接近癌症诊断,癌症诊断前的DNAmAA配对内差异显著增加,并且这种加速在诊断后持续数年。在诊断后采样的配对中,DNAmAA与Horvath模型在所有三种癌症分组中捕获癌症诊断相关的DNAmAA不同。结果表明,血液中的DNAmAA与癌症诊断有关。这可能是由于与癌症、治疗或相关的生活方式改变有关的表观遗传改变。根据目前的研究,血液中DNAmAA的生物标志物潜力似乎有限。
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来源期刊
Twin Research and Human Genetics
Twin Research and Human Genetics 医学-妇产科学
CiteScore
1.50
自引率
11.10%
发文量
37
审稿时长
6-12 weeks
期刊介绍: Twin Research and Human Genetics is the official journal of the International Society for Twin Studies. Twin Research and Human Genetics covers all areas of human genetics with an emphasis on twin studies, genetic epidemiology, psychiatric and behavioral genetics, and research on multiple births in the fields of epidemiology, genetics, endocrinology, fetal pathology, obstetrics and pediatrics. Through Twin Research and Human Genetics the society aims to publish the latest research developments in twin studies throughout the world.
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