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A checkpoint for autoreactivity in human IgM+ memory B cell development.


ABSTRACT: Autoantibodies are removed from the repertoire at two checkpoints during B cell development in the bone marrow and the periphery. Despite these checkpoints, up to 20% of the antibodies expressed by mature naive B cells in healthy humans show low levels of self-reactivity. To determine whether self-reactive antibodies are also part of the antigen-experienced memory B cell compartment, we analyzed recombinant antibodies cloned from single circulating human IgM+ memory B cells. Cells expressing antibodies specific for individual bacterial polysaccharides were expanded in the IgM+ memory compartment. In contrast, B cells expressing self-reactive and broadly bacterially reactive antibodies were removed from the repertoire in the transition from naive to IgM+ memory B cell. Selection against self-reactive antibodies was implemented before the onset of somatic hypermutation. We conclude that a third checkpoint selects against self-reactivity during IgM+ memory B cell development in humans.

SUBMITTER: Tsuiji M 

PROVIDER: S-EPMC2118214 | biostudies-literature | 2006 Feb

REPOSITORIES: biostudies-literature

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A checkpoint for autoreactivity in human IgM+ memory B cell development.

Tsuiji Makoto M   Yurasov Sergey S   Velinzon Klara K   Thomas Saskia S   Nussenzweig Michel C MC   Wardemann Hedda H  

The Journal of experimental medicine 20060130 2


Autoantibodies are removed from the repertoire at two checkpoints during B cell development in the bone marrow and the periphery. Despite these checkpoints, up to 20% of the antibodies expressed by mature naive B cells in healthy humans show low levels of self-reactivity. To determine whether self-reactive antibodies are also part of the antigen-experienced memory B cell compartment, we analyzed recombinant antibodies cloned from single circulating human IgM+ memory B cells. Cells expressing ant  ...[more]

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