T Cell Subset-specific Susceptibility to Aging

Overview

Journal Clin Immunol

Specialty Allergy & Immunology

Date 2008 Jan 29

PMID 18222733

Citations 239

Authors

Marta Czesnikiewicz-Guzik

Won-Woo Lee

Dapeng Cui

Yuko Hiruma

David L Lamar

Zhi-Zhang Yang

Joseph G Ouslander

Cornelia M Weyand

Jorg J Goronzy

Affiliations

Soon will be listed here.

Abstract

With increasing age, the competence of the immune system to fight infections and tumors declines. Age-dependent changes have been mostly described for human CD8 T cells, raising the question of whether the response patterns for CD4 T cells are different. Gene expression arrays of memory CD4 T cells yielded a similar age-induced fingerprint as has been described for CD8 T cells. In cross-sectional studies, the phenotypic changes were not qualitatively different for CD4 and CD8 T cells, but occurred much more frequently in CD8 T cells. Homeostatic stability partially explained this lesser age sensitivity of CD4 T cells. With aging, naïve and central memory CD8 T cells were lost at the expense of phenotypically distinct CD8 effector T cells, while effector CD4 T cells did not accumulate. However, phenotypic shifts on central memory T cells were also more pronounced in CD8 T cells. This distinct stability in cell surface marker expression can be reproduced in vitro. The data show that CD8 T cells are age sensitive by at least two partially independent mechanisms: fragile homeostatic control and gene expression instability in a large set of regulatory cell surface molecules.

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