2011
DOI: 10.1073/pnas.1107594108
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Nonrandom attrition of the naive CD8 + T-cell pool with aging governed by T-cell receptor:pMHC interactions

Abstract: Immunity against new infections declines in the last quartile of life, as do numbers of naive T cells. Peripheral maintenance of naive T cells over the lifespan is necessary because their production drastically declines by puberty, a result of thymic involution. We report that this maintenance is not random in advanced aging. As numbers and diversity of naive CD8 + T cells declined with aging, surviving cells underwent faster rates of homeostatic proliferation, were selected for high T-cell receptor: pMHC avid… Show more

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Cited by 133 publications
(180 citation statements)
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“…Data obtained from a variety of species (6)(7)(8)(9)(10)(11)16) indicate that the effective clonal diversity of T cells declines with age. Using CDR3 amino acid sequences obtained from the TCR b-chain (16), we estimated the age-dependent change in the effective clonal diversity of naive CD4/CD8 T cells found in human blood (Fig.…”
Section: Discussionmentioning
confidence: 99%
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“…Data obtained from a variety of species (6)(7)(8)(9)(10)(11)16) indicate that the effective clonal diversity of T cells declines with age. Using CDR3 amino acid sequences obtained from the TCR b-chain (16), we estimated the age-dependent change in the effective clonal diversity of naive CD4/CD8 T cells found in human blood (Fig.…”
Section: Discussionmentioning
confidence: 99%
“…In aged mice, the CD8 T cell repertoire is biased in favor of T cells with a high avidity for self-peptide MHC (8). These T cells preferentially undergo homeostatic proliferation, leading to a contraction of T cell repertoire diversity in aged mice (8).…”
Section: Discussionmentioning
confidence: 99%
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“…Though individual T cells bind and recognize one or at most a few epitopes via their T-cell receptor (TCR), the entire population of T cells encompasses a diverse repertoire of TCRs that, ideally, allows recognition of the epitopes on essentially any pathogen. The diversity of this repertoire declines over time, as demonstrated by experimental work in aged mice (1)(2)(3), rhesus macaques (4), and humans (5). This decline in diversity has implications for susceptibility to disease, yet, as we explore in this paper, the driving forces underlying this decline remain unclear.…”
mentioning
confidence: 93%