Ageing of the B-cell repertoire

Author:

Martin Victoria1,Wu Yu-Chang (Bryan)2,Kipling David3,Dunn-Walters Deborah1

Affiliation:

1. Division of Infection, Immunity and Inflammatory Disease, King's College London Faculty of Life Sciences & Medicine, Guys Campus, London, UK

2. Randall Division of Cell and Molecular Biophysics, King's College London Faculty of Life Sciences & Medicine, Guys Campus, London, UK

3. Institute of Cancer and Genetics, School of Medicine, Cardiff University, Heath Park, Cardiff, UK

Abstract

Older people are more susceptible to infection, less responsive to vaccination and have a more inflammatory immune environment. Using spectratype analysis, we have previously shown that the B-cell repertoire of older people shows evidence of inappropriate clonal expansions in the absence of challenge, and that this loss of B-cell diversity correlates with poor health. Studies on response to vaccination, using both spectratyping and high-throughput sequencing of the repertoire, indicate that older responses to challenge are lacking in magnitude and/or delayed significantly. Also that some of the biologically significant differences may be in different classes of antibody. We have also previously shown that normal young B-cell repertoires can vary between different phenotypic subsets of B cells. In this paper, we present an analysis of immunoglobulin repertoire in different subclasses of antibody in five different populations of B cell, and show how the repertoire in these different groups changes with age. Although some age-related repertoire differences occur in naive cells, before exogenous antigen exposure, we see indications that there is a general dysregulation of the selective forces that shape memory B-cell populations in older people.

Publisher

The Royal Society

Subject

General Agricultural and Biological Sciences,General Biochemistry, Genetics and Molecular Biology

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