TABLE 1.
Effect of caloric restriction on age-related epigenetic modifications.
| Model | Biological tissue | Impact | References | |
|---|---|---|---|---|
| Mice | Whole Tissue | Nts1 showed significantly higher expression levels within 1 month | Unnikrishnan et al. (2017) | |
| Mice | Hippocampus | Regulating DNMT3a levels, preventing age-related increases in HDAC2, and improving brain function in mice during aging | Chouliaras et al., 2011; Chouliaras et al., 2013 | |
| Female mice | Liver | Attenuates age-related methylation changes in gene promoters associated with inflammation, diabetesetc. | Hahn et al. (2017) | |
| Obese humans | _ | Short-term CR intervention leads to DNA methylation changes in genes such as ATP10A, WT1, and TNF-a, reduces lipid metabolism gene expression, and delays aging | Hahn et al. (2017) | |
| SAMP8 Mice | cerebrum | As H3K27me3 increases, aging phenomena accelerate and premature neurodegeneration develops | McCauley and Dang, (2014) | |
| Normal diploid WI-38, MRC-5 and IMR-90 human fetal lung fibroblasts | _ | Glucose restriction directly activates SIRT1, leading to chromatin remodeling of the p16INK4a gene promoter and decreased expression of this gene, and significantly prolonged cell life span | Pazin et al. (2011) | |
| C. elegans | _ | Increased H3K27 demethylase UTX-1 activity, increased expression of IIS signaling pathway genes and loss of H3K27me3 | Jin et al. (2011) | |
| Aged Mice | _ | Acetylation of histone H3 Lys9 increased | Cao et al. (2018) | |
| yeast | _ | Nαt4 expression is significantly reduced, histone H4 N-terminal acetylation is lost, and yeast lifespan is extended | Molina-Serrano et al. (2016) | |
| Mice | Serum | Elevated levels of numerous miRNAs | Dhahbi et al. (2013) | |
| Mice | cerebrum | Increases in miR-181a-1*, miR-30e, and miR-34a were counterbalanced, resulting in increased expression of Bcl-2 and decreased apoptosis | Ayyadevara et al. (2013) | |
| Aged Rats | Cerebral cortex | Increased miR-98–3p expression | Wood et al. (2015) |