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Publication : NAD<sup>+</sup> Controls Circadian Reprogramming through PER2 Nuclear Translocation to Counter Aging.

First Author  Levine DC Year  2020
Journal  Mol Cell Volume  78
Issue  5 Pages  835-849.e7
PubMed ID  32369735 Mgi Jnum  J:297101
Mgi Id  MGI:6468904 Doi  10.1016/j.molcel.2020.04.010
Citation  Levine DC, et al. (2020) NAD(+) Controls Circadian Reprogramming through PER2 Nuclear Translocation to Counter Aging. Mol Cell 78(5):835-849.e7
abstractText  Disrupted sleep-wake and molecular circadian rhythms are a feature of aging associated with metabolic disease and reduced levels of NAD(+), yet whether changes in nucleotide metabolism control circadian behavioral and genomic rhythms remains unknown. Here, we reveal that supplementation with the NAD(+) precursor nicotinamide riboside (NR) markedly reprograms metabolic and stress-response pathways that decline with aging through inhibition of the clock repressor PER2. NR enhances BMAL1 chromatin binding genome-wide through PER2(K680) deacetylation, which in turn primes PER2 phosphorylation within a domain that controls nuclear transport and stability and that is mutated in human advanced sleep phase syndrome. In old mice, dampened BMAL1 chromatin binding, transcriptional oscillations, mitochondrial respiration rhythms, and late evening activity are restored by NAD(+) repletion to youthful levels with NR. These results reveal effects of NAD(+) on metabolism and the circadian system with aging through the spatiotemporal control of the molecular clock.
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