Literature DB >> 12115615

Age- and tissue-specific differences in human germinal center B cell selection revealed by analysis of IgVH gene hypermutation and lineage trees.

Monica Banerjee1, Ramit Mehr, Alex Belelovsky, Jo Spencer, Deborah K Dunn-Walters.   

Abstract

The elderly produce increased levels of antibodies to autologous antigens and are less able to make high-affinity antibodies to foreign antigens. Ig gene hypermutation is integral to the affinity maturation process but previous studies of hypermutation with age have yielded conflicting results. The cells studied have represented post-germinal center (GC) populations and, therefore, the results may be complicated by possible differences in activation history. We studied Ig genes from GC B cells to elucidate which factors in the affinity maturation process change with age. Age-related changes in the pattern of hypermutation were seen, although the analysis of variable region heavy chain (VH) genes and their lineage trees shows that an alteration in the mechanism of somatic hypermutation is unlikely. The changes are due to founder cell effects and/or the process of selection. Striking tissue-specific differences were seen. All measurements indicated that selection of Ig genes may decrease in Peyer's patch GC but increase in splenic GC with age. These tissue-specific differences highlight the importance of considering the activation and effector sites when studying immune senescence.

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Year:  2002        PMID: 12115615     DOI: 10.1002/1521-4141(200207)32:7<1947::AID-IMMU1947>3.0.CO;2-1

Source DB:  PubMed          Journal:  Eur J Immunol        ISSN: 0014-2980            Impact factor:   5.532


  31 in total

Review 1.  Age effects on B cells and humoral immunity in humans.

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2.  Novel analysis of clonal diversification in blood B cell and bone marrow plasma cell clones in immunoglobulin light chain amyloidosis.

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3.  Ancient phylogenetic beginnings of immunoglobulin hypermutation.

Authors:  Jaroslav Kubrycht; Karel Sigler; Michal Růzicka; Pavel Soucek; Jirí Borecký; Petr Jezek
Journal:  J Mol Evol       Date:  2006-10-06       Impact factor: 2.395

4.  Older adults have a low capacity to opsonize pneumococci due to low IgM antibody response to pneumococcal vaccinations.

Authors:  Saeyoung Park; Moon H Nahm
Journal:  Infect Immun       Date:  2010-11-01       Impact factor: 3.441

5.  IGHV1, IGHV5 and IGHV7 subgroup genes in the rhesus macaque.

Authors:  Jon M Bible; Wendy Howard; Helena Robbins; Deborah K Dunn-Walters
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Review 6.  Aging affects human B cell responses.

Authors:  Daniela Frasca; Bonnie B Blomberg
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Review 7.  Effects of aging on B cell function.

Authors:  Daniela Frasca; Bonnie B Blomberg
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Review 8.  The ageing human B cell repertoire: a failure of selection?

Authors:  D K Dunn-Walters
Journal:  Clin Exp Immunol       Date:  2015-10-06       Impact factor: 4.330

9.  B-cell diversity decreases in old age and is correlated with poor health status.

Authors:  Kate L Gibson; Yu-Chang Wu; Yvonne Barnett; Orla Duggan; Robert Vaughan; Elli Kondeatis; Bengt-Olof Nilsson; Anders Wikby; David Kipling; Deborah K Dunn-Walters
Journal:  Aging Cell       Date:  2008-11-05       Impact factor: 9.304

10.  Mechanisms of immunosenescence.

Authors:  Calogero Caruso; Silvio Buffa; Giuseppina Candore; Giuseppina Colonna-Romano; Deborah Dunn-Walters; David Kipling; Graham Pawelec
Journal:  Immun Ageing       Date:  2009-07-22       Impact factor: 6.400

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