Antibody Affinity Shapes the Choice between Memory and Germinal Center B Cell Fates | Zendy

Charlotte Viant | Zendy; Georg H.J. Weymar | Zendy; Amelia Escolano | Zendy; Spencer T. Chen | Zendy; Harald Hartweger | Zendy; Melissa Cipolla | Zendy; Anna Gazumyan | Zendy; Michel C. Nussenzweig | Zendy

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Antibody Affinity Shapes the Choice between Memory and Germinal Center B Cell Fates

Author(s) -

Charlotte Viant,

Georg H.J. Weymar,

Amelia Escolano,

Spencer T. Chen,

Harald Hartweger,

Melissa Cipolla,

Anna Gazumyan,

Michel C. Nussenzweig

Publication year - 2020

Publication title -

cell

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 26.304

H-Index - 776

eISSN - 1097-4172

pISSN - 0092-8674

DOI - 10.1016/j.cell.2020.09.063

Subject(s) - biology , germinal center , antibody , memory b cell , affinity maturation , b cell , microbiology and biotechnology , immunology , genetics

Immunological memory is required for protection against repeated infections and is the basis of all effective vaccines. Antibodies produced by memory B cells play an essential role in many of these responses. We have combined lineage tracing with antibody cloning from single B cells to examine the role of affinity in B cell selection into germinal centers (GCs) and the memory B cell compartment in mice immunized with an HIV-1 antigen. We find that contemporaneously developing memory and GC B cells differ in their affinity for antigen throughout the immune response. Whereas GC cells and their precursors are enriched in antigen binding, memory B cells are not. Thus, the polyclonal memory B cell compartment is composed of B cells that were activated during the immune response but whose antigen binding affinity failed to support further clonal expansion in the GC.

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