Open AccessReversal of epigenetic aging and immunosenescent trends in humans
Author(s) -
Fahy Gregory M.,
Brooke Robert T.,
Watson James P.,
Good Zinaida,
Vasanawala Shreyas S.,
Maecker Holden,
Leipold Michael D.,
Lin David T. S.,
Kobor Michael S.,
Horvath Steve
Publication year - 2019
Publication title -
aging cell
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 3.103
H-Index - 140
eISSN - 1474-9726
pISSN - 1474-9718
DOI - 10.1111/acel.13028
Subject(s) - epigenetics , biology , biological age , demography , bioinformatics , genetics , evolutionary biology , gene , sociology
Epigenetic “clocks” can now surpass chronological age in accuracy for estimating biological age. Here, we use four such age estimators to show that epigenetic aging can be reversed in humans. Using a protocol intended to regenerate the thymus, we observed protective immunological changes, improved risk indices for many age‐related diseases, and a mean epigenetic age approximately 1.5 years less than baseline after 1 year of treatment (−2.5‐year change compared to no treatment at the end of the study). The rate of epigenetic aging reversal relative to chronological age accelerated from −1.6 year/year from 0–9 month to −6.5 year/year from 9–12 month. The GrimAge predictor of human morbidity and mortality showed a 2‐year decrease in epigenetic vs. chronological age that persisted six months after discontinuing treatment. This is to our knowledge the first report of an increase, based on an epigenetic age estimator, in predicted human lifespan by means of a currently accessible aging intervention.