Published online
doi:10.1084/jem.20071140
The Journal of Experimental Medicine, Vol. 205, No. 3, 711-723
The Rockefeller University Press, 0022-1007 $30.00
© Yager et al.
Age-associated decline in T cell repertoire diversity leads to holes in the repertoire and impaired immunity to influenza virus
Eric J. Yager,
Mushtaq Ahmed,
Kathleen Lanzer,
Troy D. Randall,
David L. Woodland, and
Marcia A. Blackman
The Trudeau Institute, Saranac Lake, NY 12983
CORRESPONDENCE Marcia A. Blackman: mblackman{at}trudeauinstitute.org
A diverse T cell repertoire is essential for a vigorous immune response to new infections, and decreasing repertoire diversity has been implicated in the age-associated decline in CD8 T cell immunity. In this study, using the well-characterized mouse influenza virus model, we show that although comparable numbers of CD8 T cells are elicited in the lung and lung airways of young and aged mice after de novo infection, a majority of aged mice exhibit profound shifts in epitope immunodominance and restricted diversity in the TCR repertoire of responding cells. A preferential decline in reactivity to viral epitopes with a low naive precursor frequency was observed, in some cases leading to "holes" in the T cell repertoire. These effects were also seen in young thymectomized mice, consistent with the role of the thymus in maintaining naive repertoire diversity. Furthermore, a decline in repertoire diversity generally correlated with impaired responses to heterosubtypic challenge. This study formally demonstrates in a mouse infection model that naturally occurring contraction of the naive T cell repertoire can result in impaired CD8 T cell responses to known immunodominant epitopes and decline in heterosubtypic immunity. These observations have important implications for the design of vaccine strategies for the elderly.
Abbreviations used: BAL, bronchoalveolar lavage; NP, NP366-374/Db; PA, PA224-233/Db.

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