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Perspectives
Homeostatic and Maturation-associated Proliferation in the Peripheral B-Cell Compartment
Menno C. van Zelm, Mirjam van der Burg and Jacques J.M. van Dongen
volume 6 | issue 23
1 December 2007Pages: 2890 - 2895
This is an open-access article
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B lymphocytes contribute to the immune system by the production of antigen-specific antibodies. When naive mature B-lymphocytes recognize antigen with their specific Ig receptors, they will undergo clonal proliferation and differentiation, thereby generating a large number of long-lived memory B cells and plasma cells that produce and secrete antigen-specific antibodies. Recently, we generated new insights on the peripheral B-cell compartment in mice and man, supported by the introduction of a novel molecular assay that quantifies the replication history of B lymphocytes. Our data indicate that naive mature B lymphocytes are able to undergo antigen-independent homeostatic proliferation. Furthermore, the extent of proliferation differs substantially between T-cell dependent and T-cell independent B-cell responses. Thus, three unique proliferation stages occur in the peripheral B-cell compartment. Now that we have identified the B-cell subsets that undergo proliferation, it is a challenge to investigate the initiation and regulation of the proliferation processes. To support the understanding of each of the three proliferation stages, we present our view on the impact of the different proliferation stages on B-cell maturation, the potential molecular mechanisms underlying these processes, and the potential implications in human immunological diseases.
Authors
Menno C. van Zelm
Erasmus MC; Rotterdam, The Netherlands
Mirjam van der Burg
Erasmus MC; Rotterdam, The Netherlands
Jacques J.M. van Dongen
Erasmus MC; Rotterdam, The Netherlands
This is an open-access article
If the document does not open, please right-click on the link (control-click on a Macintosh) and select the option to save the file to disk.




