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Vaccination-induced changes in human B-cell repertoire and pneumococcal IgM and IgA antibody at different ages

It is well known that older people are more susceptible to morbidity and mortality from infectious diseases, particularly from pulmonary diseases such as pneumococcal pneumonia where vaccines do not provide efficient protection as in younger populations. We have previously shown that the B-cell repe...

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Autores principales: Ademokun, Alexander, Wu, Yu-Chang, Martin, Victoria, Mitra, Rajive, Sack, Ulrich, Baxendale, Helen, Kipling, David, Dunn-Walters, Deborah K
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Blackwell Publishing Ltd 2011
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3264704/
https://www.ncbi.nlm.nih.gov/pubmed/21726404
http://dx.doi.org/10.1111/j.1474-9726.2011.00732.x
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author Ademokun, Alexander
Wu, Yu-Chang
Martin, Victoria
Mitra, Rajive
Sack, Ulrich
Baxendale, Helen
Kipling, David
Dunn-Walters, Deborah K
author_facet Ademokun, Alexander
Wu, Yu-Chang
Martin, Victoria
Mitra, Rajive
Sack, Ulrich
Baxendale, Helen
Kipling, David
Dunn-Walters, Deborah K
author_sort Ademokun, Alexander
collection PubMed
description It is well known that older people are more susceptible to morbidity and mortality from infectious diseases, particularly from pulmonary diseases such as pneumococcal pneumonia where vaccines do not provide efficient protection as in younger populations. We have previously shown that the B-cell repertoire in the old is reduced and hypothesise that this may contribute to the impaired humoral responses of the elderly. Here, we investigated the repertoire and antibody responses to winter vaccination in two age groups, aged 18–49 and 65–89. We found that the serum IgM and IgA pneumococcal responses were significantly impaired in the older group, with no difference in IgG levels. IGHM spectratype analysis seems to be the most promising in terms of its predictive ability for vaccine responses. Spectratypes showed a clear change in the repertoire at day 7 after vaccination, with a return to the baseline levels at day 28. The changes at day 7 reflected expansion of IGH sequences that have smaller, more hydrophilic, CDR3 regions, and these changes were attenuated in the older group. The older group was more likely to have spectratypes indicative of a reduced diversity at day 0 and day 28. On average, the baseline repertoire in the older group was comprised of larger CDR3 regions than in the younger group. In conclusion, IgA and IgM responses are significantly impaired in the elderly pneumococcal response and are likely key mediators of protection. Hydrophilicity and/or small size of the IGH CDR3 appear to be important in these responses.
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spelling pubmed-32647042012-01-24 Vaccination-induced changes in human B-cell repertoire and pneumococcal IgM and IgA antibody at different ages Ademokun, Alexander Wu, Yu-Chang Martin, Victoria Mitra, Rajive Sack, Ulrich Baxendale, Helen Kipling, David Dunn-Walters, Deborah K Aging Cell Original Articles It is well known that older people are more susceptible to morbidity and mortality from infectious diseases, particularly from pulmonary diseases such as pneumococcal pneumonia where vaccines do not provide efficient protection as in younger populations. We have previously shown that the B-cell repertoire in the old is reduced and hypothesise that this may contribute to the impaired humoral responses of the elderly. Here, we investigated the repertoire and antibody responses to winter vaccination in two age groups, aged 18–49 and 65–89. We found that the serum IgM and IgA pneumococcal responses were significantly impaired in the older group, with no difference in IgG levels. IGHM spectratype analysis seems to be the most promising in terms of its predictive ability for vaccine responses. Spectratypes showed a clear change in the repertoire at day 7 after vaccination, with a return to the baseline levels at day 28. The changes at day 7 reflected expansion of IGH sequences that have smaller, more hydrophilic, CDR3 regions, and these changes were attenuated in the older group. The older group was more likely to have spectratypes indicative of a reduced diversity at day 0 and day 28. On average, the baseline repertoire in the older group was comprised of larger CDR3 regions than in the younger group. In conclusion, IgA and IgM responses are significantly impaired in the elderly pneumococcal response and are likely key mediators of protection. Hydrophilicity and/or small size of the IGH CDR3 appear to be important in these responses. Blackwell Publishing Ltd 2011-12 /pmc/articles/PMC3264704/ /pubmed/21726404 http://dx.doi.org/10.1111/j.1474-9726.2011.00732.x Text en © 2011 The Authors. Aging Cell © 2011 Blackwell Publishing Ltd/Anatomical Society of Great Britain and Ireland http://creativecommons.org/licenses/by/2.5/ Re-use of this article is permitted in accordance with the Creative Commons Deed, Attribution 2.5, which does not permit commercial exploitation.
spellingShingle Original Articles
Ademokun, Alexander
Wu, Yu-Chang
Martin, Victoria
Mitra, Rajive
Sack, Ulrich
Baxendale, Helen
Kipling, David
Dunn-Walters, Deborah K
Vaccination-induced changes in human B-cell repertoire and pneumococcal IgM and IgA antibody at different ages
title Vaccination-induced changes in human B-cell repertoire and pneumococcal IgM and IgA antibody at different ages
title_full Vaccination-induced changes in human B-cell repertoire and pneumococcal IgM and IgA antibody at different ages
title_fullStr Vaccination-induced changes in human B-cell repertoire and pneumococcal IgM and IgA antibody at different ages
title_full_unstemmed Vaccination-induced changes in human B-cell repertoire and pneumococcal IgM and IgA antibody at different ages
title_short Vaccination-induced changes in human B-cell repertoire and pneumococcal IgM and IgA antibody at different ages
title_sort vaccination-induced changes in human b-cell repertoire and pneumococcal igm and iga antibody at different ages
topic Original Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3264704/
https://www.ncbi.nlm.nih.gov/pubmed/21726404
http://dx.doi.org/10.1111/j.1474-9726.2011.00732.x
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