| Literature DB >> 35528547 |
Haik Mkhikian1, Ken L Hayama2, Khachik Khachikyan3, Carey Li3, Raymond W Zhou3, Judy Pawling4, Suzi Klaus2, Phuong Q N Tran3, Kim M Ly3, Andrew D Gong3, Hayk Saryan3, Jasper L Hai3, David Grigoryan3, Philip L Lee3, Barbara L Newton3, Manuela Raffatellu2,5,6, James W Dennis4,7, Michael Demetriou2,3.
Abstract
Impaired T cell immunity with aging increases mortality from infectious disease. The branching of Asparagine-linked glycans is a critical negative regulator of T cell immunity. Here we show that branching increases with age in females more than males, in naïve more than memory T cells, and in CD4+ more than CD8+ T cells. Female sex hormones and thymic output of naïve T cells (TN) decrease with age, however neither thymectomy nor ovariectomy altered branching. Interleukin-7 (IL-7) signaling was increased in old female more than male mouse TN cells, and triggered increased branching. N-acetylglucosamine, a rate-limiting metabolite for branching, increased with age in humans and synergized with IL-7 to raise branching. Reversing elevated branching rejuvenated T cell function and reduced severity of Salmonella infection in old female mice. These data suggest sex-dimorphic antagonistic pleiotropy, where IL-7 initially benefits immunity through TN maintenance but inhibits TN function by raising branching synergistically with age-dependent increases in N-acetylglucosamine.Entities:
Keywords: Immunosenescence; N-acetyglucosamine; N-glycan branching; N-glycosylation; T cell, infection; aging; immunity; interleukin-7
Year: 2022 PMID: 35528547 PMCID: PMC9075523 DOI: 10.1038/s43587-022-00187-y
Source DB: PubMed Journal: Nat Aging ISSN: 2662-8465