Short-term calorie restriction ameliorates genomewide, age-related alterations in DNA methylation

被引:43
作者
Kim, Chul Hong [1 ]
Lee, Eun Kyeong [2 ]
Choi, Yeon Ja [2 ]
An, Hye Jin [2 ]
Jeong, Hyeong Oh [2 ]
Park, Daeui [3 ]
Kim, Byoung Chul [3 ]
Yu, Byung Pal [4 ]
Bhak, Jong [5 ]
Chung, Hae Yung [2 ,5 ]
机构
[1] Genomictree Inc, Daejeon, South Korea
[2] Pusan Natl Univ, Coll Pharm, Mol Inflammat Res Ctr Aging Intervent MRCA, Busandaehak Ro 63beon Gil, Busan 46241, South Korea
[3] Korea Inst Toxicol, Dept Predict Toxicol, Daejeon, South Korea
[4] Univ Texas San Antonio, Hlth Sci Ctr, Dept Physiol, San Antonio, TX 78284 USA
[5] Ulsan Natl Inst Sci & Technol, Biomed Engn, Ulsan, South Korea
基金
新加坡国家研究基金会;
关键词
aging; Bioinformatics; calorie restriction; DNA methylation; MeDIP-Seq; INFLAMMATION HYPOTHESIS; PROMOTER METHYLATION; EPIGENETIC CONTROL; TUMOR-SUPPRESSOR; OXIDATIVE STRESS; DISEASE; CANCER; LIVER; MODULATION; EXPRESSION;
D O I
10.1111/acel.12513
中图分类号
Q2 [细胞生物学];
学科分类号
071009 ; 090102 ;
摘要
DNA methylation plays major roles in many biological processes, including aging, carcinogenesis, and development. Analyses of DNA methylation using next-generation sequencing offer a new way to profile and compare methylomes across the genome in the context of aging. We explored genomewide DNA methylation and the effects of short-term calorie restriction (CR) on the methylome of aged rat kidney. Whole-genome methylation of kidney in young (6 months old), old (25 months old), and OCR (old with 4-week, short-term CR) rats was analyzed by methylated DNA immunoprecipitation and next-generation sequencing (MeDIP-Seq). CpG islands and repetitive regions were hypomethylated, but 5'-UTR, exon, and 3'-UTR hypermethylated in old and OCR rats. The methylation in the promoter and intron regions was decreased in old rats, but increased in OCR rats. Pathway enrichment analysis showed that the hypermethylated promoters in old rats were associated with degenerative phenotypes such as cancer and diabetes. The hypomethylated promoters in old rats related significantly to the chemokine signaling pathway. However, the pathways significantly enriched in old rats were not observed from the differentially methylated promoters in OCR rats. Thus, these findings suggest that short-term CR could partially ameliorate age-related methylation changes in promoters in old rats. From the epigenomic data, we propose that the hypermethylation found in the promoter regions of disease-related genes during aging may indicate increases in susceptibility to age-related diseases. Therefore, the CR-induced epigenetic changes that ameliorate age-dependent aberrant methylation may be important to CR's health-and life-prolonging effects.
引用
收藏
页码:1074 / 1081
页数:8
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