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Aborted germinal center reactions and B cell memory by follicular T cells specific for a B cell receptor V region peptide.


ABSTRACT: A fundamental problem in immunoregulation is how CD4(+) T cells react to immunogenic peptides derived from the V region of the BCR that are created by somatic mechanisms, presented in MHC II, and amplified to abundance by B cell clonal expansion during immunity. BCR neo Ags open a potentially dangerous avenue of T cell help in violation of the principle of linked Ag recognition. To analyze this issue, we developed a murine adoptive transfer model using paired donor B cells and CD4 T cells specific for a BCR-derived peptide. BCR peptide-specific T cells aborted ongoing germinal center reactions and impeded the secondary immune response. Instead, they induced the B cells to differentiate into short-lived extrafollicular plasmablasts that secreted modest quantities of Ig. These results uncover an immunoregulatory process that restricts the memory pathway to B cells that communicate with CD4 T cells via exogenous foreign Ag.

SUBMITTER: Heiser RA 

PROVIDER: S-EPMC3133611 | biostudies-literature | 2011 Jul

REPOSITORIES: biostudies-literature

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Aborted germinal center reactions and B cell memory by follicular T cells specific for a B cell receptor V region peptide.

Heiser Ryan A RA   Snyder Christopher M CM   St Clair James J   Wysocki Lawrence J LJ  

Journal of immunology (Baltimore, Md. : 1950) 20110527 1


A fundamental problem in immunoregulation is how CD4(+) T cells react to immunogenic peptides derived from the V region of the BCR that are created by somatic mechanisms, presented in MHC II, and amplified to abundance by B cell clonal expansion during immunity. BCR neo Ags open a potentially dangerous avenue of T cell help in violation of the principle of linked Ag recognition. To analyze this issue, we developed a murine adoptive transfer model using paired donor B cells and CD4 T cells specif  ...[more]

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