PMID: 6975306Nov 1, 1981Paper

Myelogenous production and maturation of B lymphocytes in the mouse

The Journal of Immunology : Official Journal of the American Association of Immunologists
K S LandrethJ Clagett

Abstract

Cells of the B lymphocyte lineage in young adult murine bone marrow were identified and resolved into compartments based on cell size and the expression of the mu heavy chain of IgM in the cytoplasm (cmu) or on the cell surface (smu). The proliferative status, renewal rate, and intercompartmental transit of cells through the defined compartments were determined using established protocols of in vivo tritiated thymidine (3H-TdR) administration, followed by radioautography of bone marrow smears. In addition, we specifically tested whether any of the defined cell compartments were derived from long-lived lymphocytes that are known to enter the marrow. Only large cells immediately incorporated the DNA precursor and both small cmu+ smu- and cmu+ smu+ cells were postmitotic lymphocytes. Large cmu+ smu- cells were found to be a rapid transit compartment in which the last mitosis of B lymphocyte differentiation takes place. All large cmu+ smu- cells divided only once, and both daughter cells entered the postmitotic small cmu+ smu- population. Large cmu+ smu- cells relied for their maintenance entirely on cell input from an Ig- progenitor compartment. Progenitors of cmu+ smu- large cells were not small lymphocytes, proliferated less rap...Continue Reading

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