Perspectives
Nature Reviews Immunology 6, 785-790 (October 2006) | doi:10.1038/nri1938
Opinion: B-cell memory: are subsets necessary?
David Tarlinton1 About the author
Abstract
B-cell memory is provided by populations of quiescent memory B cells and long-lived plasma cells. Whereas it is clear that both of these cell populations arise from germinal centres, the signals and circumstances that trigger germinal-centre B cells to enter and then persist in memory compartments are poorly defined. Here, I propose that germinal centres produce memory B cells and plasma cells throughout the immune response and that memory B cells arise by the emigration of B cells that are chosen at random from the pool available in the germinal centre. The ability of such emigrants to survive as memory B cells depends on their germinal-centre 'history', with the persistence of high-affinity B-cell variants being favoured.
Author affiliations
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David Tarlinton is at The Walter and Eliza Hall Institute of Medical Research, 1G Royal Parade, Parkville, VIC 3050, Australia.
Email: tarlinton@wehi.edu.au
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