The B‐cell biology of aging

Abstract

Summary: Although both the number and responsiveness of peripheral B cells in aged mice remain relatively intact, there are dramatic changes in B-cell generation. Alterations in B-cell development include both a skewing of V-gene utilization, especially in cells responsive to phosphorylcholine, and a decrease in the generation of various developmental B-cell sub-sets. The altered representation of these subsets appears to be the consequence of two developmental blocks. The first developmental block occurs during the maturation of pro-B cells and is evidenced by a decrease in the number of pre-B cells. The second developmental block occurs at the earliest stage of slg⁺-cell maturation (slgM^{very lo}). Because of this block in B-cell maturation, it spite of a decrease in incoming pre-B cells, the number of sIgM^{very lo} cells appears to increase in aged mice. Additionally, the time of residence of cells within this maturational stage increases dramatically, While the proportion of cells in more mature (sIgM^hi) stages of bone marrow development are decreased. In addition to the decreased number of maturing bone marrow B cells, the population of splenic B cells that represent recent bone marrow émigrés (HSA^{very hi}) is markedly decreased. In the face of this decrease in newly emerging cells from the bone marrow, the population of mature splenic B cells is maintained by their increased longevity.