| Literature DB >> 27742546 |
Yinyin Li1, Yi Shen1, Philipp Hohensinner2, Jihang Ju1, Zhenke Wen1, Stuart B Goodman3, Hui Zhang1, Jörg J Goronzy1, Cornelia M Weyand4.
Abstract
Immune aging manifests with a combination of failing adaptive immunity and insufficiently restrained inflammation. In patients with rheumatoid arthritis (RA), T cell aging occurs prematurely, but the mechanisms involved and their contribution to tissue-destructive inflammation remain unclear. We found that RA CD4+ T cells showed signs of aging during their primary immune responses and differentiated into tissue-invasive, proinflammatory effector cells. RA T cells had low expression of the double-strand-break repair nuclease MRE11A, leading to telomeric damage, juxtacentromeric heterochromatin unraveling, and senescence marker upregulation. Inhibition of MRE11A activity in healthy T cells induced the aging phenotype, whereas MRE11A overexpression in RA T cells reversed it. In human-synovium chimeric mice, MRE11Alow T cells were tissue-invasive and pro-arthritogenic, and MRE11A reconstitution mitigated synovitis. Our findings link premature T cell aging and tissue-invasiveness to telomere deprotection and heterochromatin unpacking, identifying MRE11A as a therapeutic target to combat immune aging and suppress dysregulated tissue inflammation.Entities:
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Year: 2016 PMID: 27742546 PMCID: PMC5123765 DOI: 10.1016/j.immuni.2016.09.013
Source DB: PubMed Journal: Immunity ISSN: 1074-7613 Impact factor: 31.745