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日本超级人瑞的表观遗传特征:一项横断面研究。

Epigenetic profile of Japanese supercentenarians: a cross-sectional study.

机构信息

Division of Biomedical Information Analysis, Iwate Medical University, Iwate, Japan; Institute for Biomedical Sciences, Iwate Medical University, Iwate, Japan.

Healthcare Medical Group, KDDI Research, Saitama, Japan.

出版信息

Lancet Healthy Longev. 2023 Feb;4(2):e83-e90. doi: 10.1016/S2666-7568(23)00002-8.

Abstract

BACKGROUND

Centenarians and supercentenarians with exceptional longevity are excellent models for research towards improvements of healthy life expectancy. Extensive research regarding the maintenance and reduction of epigenetic age has provided insights into increasing healthy longevity. To this end, we explored the epigenetic signatures reflecting hallmarks of exceptional healthy longevity, including avoidance of age-related diseases and cognitive functional decline.

METHODS

In this cross-sectional study, we enrolled Japanese non-centenarians (eligible participants aged 20-80 years) from the Tohoku Medical Megabank Community-Based Cohort Study and centenarians and supercentenarians (aged 101-115 years) from the Tokyo Centenarian Study and the Japanese Semi-supercentenarian Study. We assessed participants' whole-blood DNA methylation profiles and then developed sex-specific and non-specific first-generation epigenetic clocks by elastic net regression, calculated individuals' epigenetic ages, and assessed their age acceleration. We also screened for age-related CpG sites in non-centenarians by epigenome-wide linear regression analyses and ANOVA. We subsequently investigated which CpG sites in centenarians and supercentenarians had DNA methylation patterns following the age-related findings obtained from non-centenarians and which did not. We further characterised CpG sites with hypermethylation or hypomethylation in the centenarians and supercentenarians using enrichment and protein-protein interaction network analyses.

FINDINGS

We enrolled 421 non-centenarians (231 [55%] women and 190 [45%] men; age range 20-78 years), recruited between May 20, 2013, and March 31, 2016, and 94 centenarians and supercentenarians (66 women [70%] and 28 [30%] men; age range 101-115 years), recruited between Jan 20, 2001, and April 17, 2018. Non-sex-specific epigenetic clock showed the highest accuracy (r=0·96) based on which centenarians and supercentenarians had negative epigenetic age acceleration. Epigenome-wide association analyses further showed that centenarians and supercentenarians had younger-than-expected epigenetic states (DNA methylation profiles similar to those of non-centenarians) for 557 CpG sites enriched in cancer-related and neuropsychiatric-related genes, whereas these individuals had advanced (or older) epigenetic states for 163 CpG sites represented by genes related to TGF-β signalling, which is involved in anti-inflammatory responses and known to contribute to healthy ageing.

INTERPRETATION

These results indicate that exceptionally healthy longevity depends not only on maintaining young epigenetic states but also on advanced states of specific epigenetic regions.

FUNDING

The Japan Agency for Medical Research and Development, KDDI Research, and Keio University.

TRANSLATION

For the Japanese translation of the abstract see Supplementary Materials section.

摘要

背景

百岁老人和超级百岁老人拥有非凡的长寿,是研究提高健康预期寿命的绝佳模型。广泛的研究表明,表观遗传年龄的维持和减少可以洞察到健康长寿的增加。为此,我们探索了反映非凡健康长寿特征的表观遗传特征,包括避免与年龄相关的疾病和认知功能下降。

方法

在这项横断面研究中,我们招募了来自东北医科大学百万生物库社区队列研究的日本非百岁老人(20-80 岁符合条件的参与者)和来自东京百岁老人研究和日本半超级百岁老人研究的百岁老人和超级百岁老人(年龄 101-115 岁)。我们评估了参与者的全血 DNA 甲基化谱,然后通过弹性网络回归开发了性别特异性和非特异性第一代表观遗传时钟,计算了个体的表观遗传年龄,并评估了他们的年龄加速。我们还通过全基因组线性回归分析和 ANOVA 对非百岁老人进行了与年龄相关的 CpG 位点筛选。随后,我们研究了百岁老人和超级百岁老人中哪些 CpG 位点的 DNA 甲基化模式与非百岁老人的年龄相关发现一致,哪些不一致。我们进一步使用富集和蛋白质-蛋白质相互作用网络分析来研究百岁老人和超级百岁老人中 CpG 位点的过度甲基化或低甲基化。

结果

我们招募了 421 名非百岁老人(231 名女性[55%]和 190 名男性[45%];年龄范围 20-78 岁),于 2013 年 5 月 20 日至 2016 年 3 月 31 日招募,并招募了 94 名百岁老人和超级百岁老人(66 名女性[70%]和 28 名男性[30%];年龄范围 101-115 岁),于 2001 年 1 月 20 日至 2018 年 4 月 17 日招募。非性别特异性表观遗传时钟显示出最高的准确性(r=0.96),基于此,百岁老人和超级百岁老人的表观遗传年龄加速呈负相关。全基因组关联分析进一步表明,百岁老人和超级百岁老人的表观遗传状态比预期更年轻(与非百岁老人相似的 DNA 甲基化模式),这与癌症相关和神经精神相关基因中富集的 557 个 CpG 位点有关,而这些个体的 163 个 CpG 位点代表与 TGF-β 信号转导相关的基因表现出更先进(或更老)的表观遗传状态,该信号转导参与抗炎反应,已知有助于健康衰老。

解释

这些结果表明,非凡的健康长寿不仅取决于维持年轻的表观遗传状态,还取决于特定表观遗传区域的先进状态。

资金

日本医疗研究与发展机构、KDDI 研究和庆应义塾大学。

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