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The Journal of Immunology, 2003, 171: 6372-6380.
Copyright © 2003 by The American Association of Immunologists

B Lymphocyte Development in Rabbit: Progenitor B Cells and Waning of B Lymphopoiesis 1

Paul J. Jasper, Shi-Kang Zhai, Susan L. Kalis, Mae Kingzette and Katherine L. Knight2

Department of Microbiology and Immunology, Loyola University Chicago, Maywood, IL 60153

In mammals that use gut-associated lymphoid tissues for expansion and somatic diversification of the B cell repertoire, B lymphopoiesis occurs early in ontogeny and does not appear to continue throughout life. In these species, including sheep, rabbit, and cattle, little is known about the pathway of B cell development and the time at which B lymphopoiesis wanes. We examined rabbit bone marrow by immunofluorescence with anti-CD79a and anti-µ and identified both proB and preB cells. The proB cells represent the vast majority of B-lineage cells in the bone marrow at birth and by incorporation of 5-bromo-2'-deoxyuridine, they appear to be a dynamic population. PreB cells reach maximum levels in the bone marrow at 3 wk of age, and B cells begin to accumulate at 7 wk of age. We cloned two VpreB and one {lambda}5 gene and demonstrated that they are expressed within B-lineage cells in bone marrow. VpreB and {lambda}5 coimmunoprecipitated with the µ-chain in lysates of 293T cells transfected with VpreB, {lambda}5, and µ, indicating that VpreB, {lambda}5, and µ-chains associate in a preB cell receptor-like complex. By 16 wk of age, essentially no proB or preB cells are found in bone marrow and by PCR amplification, B cell recombination excision circles were reduced 200-fold. By 18 mo of age, B cell recombination excision circles were reduced 500- to 1000-fold. We suggest that B cell development in the rabbit occurs primarily through the classical, or ordered, pathway and show that B lymphopoiesis is reduced over 99% by 16 wk of age.




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