Literature DB >> 24805232

Clonal selection in the germinal centre by regulated proliferation and hypermutation.

Alexander D Gitlin1, Ziv Shulman1, Michel C Nussenzweig2.   

Abstract

During immune responses, B lymphocytes clonally expand and undergo secondary diversification of their immunoglobulin genes in germinal centres (GCs). High-affinity B cells are expanded through iterative interzonal cycles of division and hypermutation in the GC dark zone followed by migration to the GC light zone, where they are selected on the basis of affinity to return to the dark zone. Here we combine a transgenic strategy to measure cell division and a photoactivatable fluorescent reporter to examine whether the extent of clonal expansion and hypermutation are regulated during interzonal GC cycles. We find that both cell division and hypermutation are directly proportional to the amount of antigen captured and presented by GC B cells to follicular helper T cells in the light zone. Our data explain how GC B cells with the highest affinity for antigen are selectively expanded and diversified.

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Year:  2014        PMID: 24805232      PMCID: PMC4271732          DOI: 10.1038/nature13300

Source DB:  PubMed          Journal:  Nature        ISSN: 0028-0836            Impact factor:   49.962


  30 in total

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7.  Rapid methods for the analysis of immunoglobulin gene hypermutation: application to transgenic and gene targeted mice.

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  239 in total

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5.  B Cell Receptor Crosslinking Augments Germinal Center B Cell Selection when T Cell Help Is Limiting.

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Review 8.  Strategies to guide the antibody affinity maturation process.

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9.  Germinal center reaction: antigen affinity and presentation explain it all.

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10.  The Transcription Factor AP4 Mediates Resolution of Chronic Viral Infection through Amplification of Germinal Center B Cell Responses.

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