Integrative epigenomic and transcriptomic analyses reveal metabolic switching by intermittent fasting in brain

Authors
Ng, Gavin Yong-QuanSheng, Dominic Paul Lee KokBae, Han-GyuKang, Sung WookFann, David Yang-WeiPark, JinsuKim, JoonkiAlli-Shaik, AsfaLee, JeongmiKim, EunaePark, SunyoungHan, Jeung-WhanKaramyan, VardanOkun, EitanDheen, ThameemHande, Manoor PrakashVemuganti, RaghuMallilankaraman, KarthikLim, Lina H. K.Kennedy, Brian K.Drummond, Grant R.Sobey, Christopher G.Gunaratne, JayanthaMattson, Mark P.Foo, Roger Sik-YinJo, Dong-GyuArumugam, Thiruma V.
Issue Date
2022-08
Publisher
SPRINGER
Citation
Geroscience, v.44, pp.2171 - 2194
Abstract
Intermittent fasting (IF) remains the most effective intervention to achieve robust anti-aging effects and attenuation of age-related diseases in various species. Epigenetic modifications mediate the biological effects of several environmental factors on gene expression; however, no information is available on the effects of IF on the epigenome. Here, we first found that IF for 3 months caused modulation of H3K9 trimethylation (H3K9me(3)) in the cerebellum, which in turn orchestrated a plethora of transcriptomic changes involved in robust metabolic switching processes commonly observed during IF. Second, a portion of both the epigenomic and transcriptomic modulations induced by IF was remarkably preserved for at least 3 months post-IF refeeding, indicating that memory of IF-induced epigenetic changes was maintained. Notably, though, we found that termination of IF resulted in a loss of H3K9me(3) regulation of the transcriptome. Collectively, our study characterizes the novel effects of IF on the epigenetic-transcriptomic axis, which controls myriad metabolic processes. The comprehensive analyses undertaken in this study reveal a molecular framework for understanding how IF impacts the metabolo-epigenetic axis of the brain and will serve as a valuable resource for future research.
Keywords
WEB SERVER; EXPRESSION; METHYLATION; HOMEOSTASIS; GENERATION; OXIDATION; H3K9ME3; MUSCLE; MEMORY; Cerebellum; Epigenetics; Intermittent fasting; Metabolism; Transcriptomics
ISSN
2509-2715
URI
https://pubs.kist.re.kr/handle/201004/114854
DOI
10.1007/s11357-022-00537-z
Appears in Collections:
KIST Article > 2022
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