bcl-2 Transgene Expression Inhibits Apoptosis in the Germinal Center and Reveals Differences in the Selection of Memory B Cells and Bone Marrow Antibody-forming Cells

doi:10.1084/jem.191.3.475

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© The Rockefeller University Press, 0022-1007/2000/2/475/ $5.00
The Journal of Experimental Medicine, Volume 191, Number 3, February 7, 2000 475-484

Original Article

bcl-2 Transgene Expression Inhibits Apoptosis in the Germinal Center and Reveals Differences in the Selection of Memory B Cells and Bone Marrow Antibody-forming Cells

Kenneth G.C. Smith^b, Amanda Light^a, Lorraine A. O'Reilly^a, Soon-Meng Ang^a, Andreas Strasser^a, and David Tarlinton^a
^a The Walter and Eliza Hall Institute of Medical Research, Post Office Royal Melbourne Hospital, Victoria 3050, Australia
^b Cambridge Institute for Medical Research and the Department of Medicine, University of Cambridge School of Clinical Medicine, Cambridge CB2 2QQ, United Kingdom

Correspondence to: David Tarlinton, The Walter and Eliza Hall Institute, PO Royal Melbourne Hospital, Victoria 3050, Australia. Tel:61-3-9345-2615 Fax:61-3-9347-0852 E-mail:tarlinton{at}wehi.edu.au.

Immunization with T cell–dependent antigens generateslong-lived memory B cells and antibody-forming cells (AFCs).Both populations originate in germinal centers and, predominantly,produce antibodies with high affinity for antigen. The meansby which germinal center B cells are recruited into these populationsremains unclear. We have examined affinity maturation of antigen-specificB cells in mice expressing the cell death inhibitor bcl-2 asa transgene. Such mice had reduced apoptosis in germinal centersand an excessive number of memory B cells with a low frequencyof V gene somatic mutation, including those mutations encodingamino acid exchanges known to enhance affinity. Despite thefrequency of AFCs being increased in bcl-2–transgenicmice, the fraction secreting high-affinity antibody in the bonemarrow at day 42 remained unchanged compared with controls.The inability of BCL-2 to alter selection of bone marrow AFCsis consistent with these cells being selected within the germinalcenter on the basis of their affinity being above some thresholdrather than their survival being due to a selective competitionfor an antigen-based signal. Continuous competition for antigendoes, however, explain formation of the memory compartment.

Key Words: affinity maturation, B cell, immunologic memory, plasma cell,somatic mutation

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