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经典人类单核细胞的增强表观遗传学分析揭示了 DNA 甲基组中健康衰老的特定特征。

Enhanced epigenetic profiling of classical human monocytes reveals a specific signature of healthy aging in the DNA methylome.

机构信息

Department of Pathology and Immunology, Washington University School of Medicine, Saint Louis, MO, USA.

These authors contributed equally: Irina Shchukina, Juhi Bagaitkar, Oleg Shpynov.

出版信息

Nat Aging. 2021 Jan;1(1):124-141. doi: 10.1038/s43587-020-00002-6. Epub 2020 Nov 23.

Abstract

The impact of healthy aging on molecular programming of immune cells is poorly understood. Here, we report comprehensive characterization of healthy aging in human classical monocytes, with a focus on epigenomic, transcriptomic, and proteomic alterations, as well as the corresponding proteomic and metabolomic data for plasma, using healthy cohorts of 20 young and 20 older males (~27 and ~64 years old on average). For each individual, we performed eRRBS-based DNA methylation profiling, which allowed us to identify a set of age-associated differentially methylated regions (DMRs) - a novel, cell-type specific signature of aging in DNA methylome. Hypermethylation events were associated with H3K27me3 in the CpG islands near promoters of lowly-expressed genes, while hypomethylated DMRs were enriched in H3K4me1 marked regions and associated with age-related increase of expression of the corresponding genes, providing a link between DNA methylation and age-associated transcriptional changes in primary human cells.

摘要

健康衰老对免疫细胞分子编程的影响还知之甚少。在这里,我们报告了对人类经典单核细胞健康衰老的全面描述,重点研究了表观基因组、转录组和蛋白质组的改变,以及使用 20 名年轻男性和 20 名老年男性(平均年龄分别约为 27 岁和 64 岁)的健康队列进行的血浆相应蛋白质组学和代谢组学数据。对于每个个体,我们进行了基于 eRRBS 的 DNA 甲基化分析,这使我们能够确定一组与年龄相关的差异甲基化区域(DMR)——在 DNA 甲基组中,这是一种新型的、细胞类型特异性的衰老特征。CpG 岛中启动子附近的高甲基化事件与低表达基因的 H3K27me3 相关,而低甲基化 DMR 则富含 H3K4me1 标记区域,并与相应基因的年龄相关表达增加相关,为 DNA 甲基化与原代人类细胞中与年龄相关的转录变化之间提供了联系。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c0d8/8597198/cbfeed24f841/nihms-1635539-f0008.jpg

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