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Age-Related Changes in B Cells Relevant to Vaccine Responses

Deborah K. Dunn‐Walters, Alexander T. Stewart, Emma Sinclair, Ilaria Serangeli

2020Interdisciplinary topics in gerontology and geriatrics16 citationsDOI

Abstract

Older people have reduced immune responses to infection and vaccination. B cell activation is key for the efficacy of the vaccine response, but there are several age-related changes in B cells which may contribute to the loss of vaccine efficacy. Different subpopulations of B cells have different functions and phenotypes. These populations can change as we age; older people have been shown to have fewer "IgM memory" cells, regulatory B cells and plasma cells and more IgD-CD27- "double-negative" and "age-related B cells." While the overall quantity of antibody in the blood does not change, the quality of the B cell response changes; producing less specific antibodies upon challenge and more autoreactive antibodies. This could be due to changes in selection pressures, as has been demonstrated by repertoire sequencing of different subsets of B cells at different ages. Other changes in antibody repertoire are seen, including greater levels of IgG2 in older people and altered IgG1 IGHV gene usage. Since B cells rely on their environment for efficient responses, some of these changes may be due to age-related changes in accessory cells/signals. Other changes appear to be intrinsic to older/aged B cells themselves, such as their tendency to produce greater levels of inflammatory cytokines.

Topics & Concepts

ImmunologyAntibodyImmune systemBiologyMemory B cellImmunoglobulin DB cellPhenotypeB-1 cellIGHV@VaccinationRepertoireGeneT cellGeneticsAntigen-presenting cellAcousticsLeukemiaPhysicsChronic lymphocytic leukemiaT-cell and B-cell ImmunologyImmunotherapy and Immune ResponsesImmune Cell Function and Interaction
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