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Department of Microbiology and Immunology, University of Maryland School of Medicine, Baltimore, MD 21201
The primary burst of Ab and germinal center (GC) formation in
response to T-dependent Ag is compromised in aging mice. Here we
examine the effects of aging on the post-GC phase of memory B cell
differentiation and the late Ab repertoire maturation in bone marrow
(BM) in mice immunized with a hapten nitrophenyl coupled to chicken
-globulin. Specific Ab-forming cells (AFC) with mutated
VH genes accumulated preferentially in the BM of aged mice,
although the AFC numbers and average number of mutations per
VH were lower, and the D gene usage was less restricted
compared with those in the young animals. However, the repertoire of
AFC after an Ag boost demonstrated the hallmarks of Ag selection,
including the recurrent mutations and canonical VD rearrangements,
similar to the late primary response in young animals. It is
postulated that the Ab repertoire maturation in aged mice is delayed
and may be notably improved by repeated
immunizations.
This article has been cited by other articles:
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  J. E. Labrie III, A. P. Sah, D. M. Allman, M. P. Cancro, and R. M. Gerstein Bone Marrow Microenvironmental Changes Underlie Reduced RAG-mediated Recombination and B Cell Generation in Aged Mice J. Exp. Med., August 16, 2004; 200(4): 411 - 423. [Abstract] [Full Text] [PDF]
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