Literature DB >> 22246631

Defective CD8 T cell responses in aged mice are due to quantitative and qualitative changes in virus-specific precursors.

Vilma Decman1, Brian J Laidlaw, Travis A Doering, Jin Leng, Hildegund C J Ertl, Daniel R Goldstein, E John Wherry.   

Abstract

Aging is associated with suboptimal CD8 T cell responses to viral infections. It is not clear whether these poor responses are due to environmental influences or quantitative and qualitative changes in the pool of responding CD8 T cells. Our studies demonstrated several deleterious age-related changes in the pool of Ag-specific CD8 T cells that respond to infection. The majority of CD8 T cells from uninfected aged mice was CD44(Hi) and had increased expression of inhibitory receptors including PD1, LAG3, 2B4, and CD160. These aged CD44(Hi) CD8 T cells were transcriptionally similar to exhausted CD8 T cells found during chronic infections. In addition, the number of virus-specific precursors in aged mice prior to infection was decreased up to 10-fold, and many of these Ag-specific precursors had high expression of CD44 and PD1. Finally, TCR transgenic studies demonstrated that the CD44(Hi) Ag-specific CD8 T cells from unimmunized aged and young mice were qualitatively inferior compared with CD44(Lo) CD8 T cells from aged or young donors. Thus, a decrease in precursor frequency as well as qualitative changes of CD8 T cells during aging are directly related to impaired immunity.

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Year:  2012        PMID: 22246631      PMCID: PMC3320034          DOI: 10.4049/jimmunol.1101098

Source DB:  PubMed          Journal:  J Immunol        ISSN: 0022-1767            Impact factor:   5.422


  55 in total

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3.  Aging in the context of immunological architecture, function and disease outcomes.

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4.  Endogenous naive CD8+ T cell precursor frequency regulates primary and memory responses to infection.

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5.  The generation of protective memory-like CD8+ T cells during homeostatic proliferation requires CD4+ T cells.

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7.  Identification of two major types of age-associated CD8 clonal expansions with highly divergent properties.

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  60 in total

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Authors:  Philipp J Hohensinner; Jörg J Goronzy; Cornelia M Weyand
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3.  Cutting Edge: The Aging Immune System Reveals the Biological Impact of Direct Antigen Presentation on CD8 T Cell Responses.

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4.  Role of Cell-Intrinsic and Environmental Age-Related Changes in Altered Maintenance of Murine T Cells in Lymphoid Organs.

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6.  Aging promotes acquisition of naive-like CD8+ memory T cell traits and enhanced functionalities.

Authors:  Jens Eberlein; Bennett Davenport; Tom Nguyen; Francisco Victorino; Kelsey Haist; Kevin Jhun; Anis Karimpour-Fard; Lawrence Hunter; Ross Kedl; Eric T Clambey; Dirk Homann
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7.  Two separate defects affecting true naive or virtual memory T cell precursors combine to reduce naive T cell responses with aging.

Authors:  Kristin R Renkema; Gang Li; Angela Wu; Megan J Smithey; Janko Nikolich-Žugich
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8.  Increased T-bet is associated with senescence of influenza virus-specific CD8 T cells in aged humans.

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Review 10.  Understanding immunosenescence to improve responses to vaccines.

Authors:  Jörg J Goronzy; Cornelia M Weyand
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