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Title: Increased DNA methylation, cellular senescence and premature epigenetic aging in guinea pigs and humans with tuberculosis.

Authors: Bobak, Carly A; Abhimanyu; Natarajan, Harini; Gandhi, Tanmay; Grimm, Sandra L; Nishiguchi, Tomoki; Koster, Kent; Longlax, Santiago Carrero; Dlamini, Qiniso; Kahari, Jacquiline; Mtetwa, Godwin; Cirillo, Jeffrey D; O'Malley, James; Hill, Jane E; Coarfa, Cristian; DiNardo, Andrew R

Published In Aging (Albany NY), (2022 Mar 07)

Abstract: BACKGROUND: Tuberculosis (TB) is the archetypical chronic infection, with patients having months of symptoms before diagnosis. In the two years after successful therapy, survivors of TB have a three-fold increased risk of death. METHODS: Guinea pigs were infected with Mycobacterium tuberculosis (Mtb) for 45 days, followed by RRBS DNA methylation analysis. In humans, network analysis of differentially expressed genes across three TB cohorts were visualized at the pathway-level. Serum levels of inflammation were measured by ELISA. Horvath (DNA methylation) and RNA-seq biological clocks were used to investigate shifts in chronological age among humans with TB. RESULTS: Guinea pigs with TB demonstrated DNA hypermethylation and showed system-level similarity to humans with TB (p-value = 0.002). The transcriptome in TB in multiple cohorts was enriched for DNA methylation and cellular senescence. Senescence associated proteins CXCL9, CXCL10, and TNF were elevated in TB patients compared to healthy controls. Humans with TB demonstrate 12.7 years (95% CI: 7.5, 21.9) and 14.38 years (95% CI: 10.23-18.53) of cellular aging as measured by epigenetic and gene expression based cellular clocks, respectively. CONCLUSIONS: In both guinea pigs and humans, TB perturbs epigenetic processes, promoting premature cellular aging and inflammation, a plausible means to explain the long-term detrimental health outcomes after TB.

PubMed ID: 35256539 Exiting the NIEHS site

MeSH Terms: Animals; Cellular Senescence/genetics; DNA Methylation*; Epigenesis, Genetic; Guinea Pigs; Humans; Inflammation/genetics; Tuberculosis*/complications; Tuberculosis*/genetics

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