Abstract
Annual Review of Immunology
Vol. 23:
487-513
(Volume publication date April 2005)
(doi:10.1146/annurev.immunol.23.021704.115732)
First published online as a Review in Advance on November 29, 2004ANTIGEN-SPECIFIC MEMORY B CELL DEVELOPMENT ▪ Abstract Helper T (Th) cell–regulated B cell immunity progresses in an ordered cascade of cellular development that culminates in the production of antigen-specific memory B cells. The recognition of peptide MHC class II complexes on activated antigen-presenting cells is critical for effective Th cell selection, clonal expansion, and effector Th cell function development (Phase I). Cognate effector Th cell–B cell interactions then promote the development of either short-lived plasma cells (PCs) or germinal centers (GCs) (Phase II). These GCs expand, diversify, and select high-affinity variants of antigen-specific B cells for entry into the long-lived memory B cell compartment (Phase III). Upon antigen rechallenge, memory B cells rapidly expand and differentiate into PCs under the cognate control of memory Th cells (Phase IV). We review the cellular and molecular regulators of this dynamic process with emphasis on the multiple memory B cell fates that develop in vivo. Most recent citing papers (via CrossRef)The role of immunoglobulin E-binding epitopes in the characterization of food allergy Current Opinion in Allergy and Clinical Immunology 9(4):357-363 (2009) Plasma and memory B-cell kinetics in infants following a primary schedule of CRM
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-conjugated serogroup C meningococcal polysaccharide vaccine Immunology 127(1):134-143 (2009) Clonal dissection of the human memory B-cell repertoire following infection and vaccination European Journal of Immunology 39(5):1260-1270 (2009) Mechanisms of Alloantibody Production in Sensitized Renal Allograft Recipients American Journal of Transplantation 9(5):998-1005 (2009) The function of follicular helper T cells is regulated by the strength of T cell antigen receptor binding Nature Immunology 10(4):375-384 (2009)
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