| Literature DB >> 29924995 |
Kylie M Quinn1, Annette Fox2, Kim L Harland2, Brendan E Russ3, Jasmine Li3, Thi H O Nguyen2, Liyen Loh2, Moshe Olshanksy3, Haroon Naeem4, Kirill Tsyganov4, Florian Wiede5, Rosela Webster6, Chantelle Blyth6, Xavier Y X Sng6, Tony Tiganis5, David Powell4, Peter C Doherty7, Stephen J Turner8, Katherine Kedzierska2, Nicole L La Gruta9.
Abstract
Age-associated decreases in primary CD8+ T cell responses occur, in part, due to direct effects on naive CD8+ T cells to reduce intrinsic functionality, but the precise nature of this defect remains undefined. Aging also causes accumulation of antigen-naive but semi-differentiated "virtual memory" (TVM) cells, but their contribution to age-related functional decline is unclear. Here, we show that TVM cells are poorly proliferative in aged mice and humans, despite being highly proliferative in young individuals, while conventional naive T cells (TN cells) retain proliferative capacity in both aged mice and humans. Adoptive transfer experiments in mice illustrated that naive CD8 T cells can acquire a proliferative defect imposed by the aged environment but age-related proliferative dysfunction could not be rescued by a young environment. Molecular analyses demonstrate that aged TVM cells exhibit a profile consistent with senescence, marking an observation of senescence in an antigenically naive T cell population.Entities:
Keywords: CD8(+) T cells; T cell dysfunction; aging; cellular senescence; exhaustion; naive CD8(+) T cells; virtual memory T cells
Year: 2018 PMID: 29924995 DOI: 10.1016/j.celrep.2018.05.057
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423