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Literature DB >> 24405293

A population biological approach to understanding the maintenance and loss of the T-cell repertoire during aging.

Philip L F Johnson¹, Jörg J Goronzy, Rustom Antia.

Abstract

The adaptive immune system requires a diverse T-cell repertoire to be able to respond to a wide variety of pathogens. Worryingly, the repertoire diversity declines dramatically in old age. As thymic output generates novel T cells, the conventional view holds that a decrease in this output with age is responsible for the loss in the repertoire. However, many additional factors affect the repertoire such as homeostatic turnover and antigen-dependent expansion in response to infection. Mathematical models taking a population biology perspective are important tools for understanding how the interplay between these factors affects the immune repertoire. These models suggest that thymic decline is not a major factor but rather that some combination of virus-induced proliferation and T-cell-intrinsic genetic or epigenetic changes gives rise to the oligoclonal expansions that cause the decline in T-cell diversity. We also discuss consequences for strategies to rejuvenate the immune repertoire in old age.

Keywords: T-cell receptors; memory; repertoire evolution

Mesh：

Year: 2014 PMID： 24405293 PMCID： PMC4008225 DOI： 10.1111/imm.12244

Source DB: PubMed Journal: Immunology ISSN： 0019-2805 Impact factor: 7.397

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