1. Expression of cell surface markers after human B lymphocyte activation
- Author
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Stuart F. Schlossman, Philip Stashenko, Russell Hardy, and Lee M. Nadler
- Subjects
Cytoplasm ,Lymphoid Tissue ,Cellular differentiation ,Immunoglobulins ,Spleen ,Lymphocyte Activation ,Antigen ,medicine ,Humans ,Tissue Distribution ,Antibody-Producing Cells ,B-Lymphocytes ,Multidisciplinary ,biology ,Cluster of differentiation ,Pokeweed mitogen ,Cell Differentiation ,Molecular biology ,Phenotype ,Lymphatic system ,medicine.anatomical_structure ,Pokeweed Mitogens ,Antigens, Surface ,Immunology ,biology.protein ,Lymph ,Antibody ,Research Article - Abstract
The fate of two recently described human B lymphocyte-specific antigens (B1 and B2) was studied after B-cell activation in vivo and in vitro. Whereas both B1 and B2 were present on virtually all B cells from normal lymph nodes, B2 was absent from approximately 50% of B cells from hyperplastic lymph nodes. When B cells from spleen, tonsil, or peripheral blood were stimulated in vitro with pokeweed mitogen, activated cells were found to lose B2 (days 4-5) and subsequently B1 (days 6-7). Temporally, B2 loss was accompanied by loss of surface IgD, expression of T10, and the development of intracytoplasmic IgM; B1 loss was correlated with the acquisition of surface IgG and the appearance of intracytoplasmic IgG. Peripheral blood B cells, on which B2 is normally only weakly expressed (B1++++B2+) in contrast to B cells from secondary lymphoid organs (B1++++B2++), exhibited a transitory increase in B2 expression to the B1++++B2++ phenotype prior to B2 disappearance during activation. Taken together with other findings, this observation suggests that peripheral blood may contain a relatively immature subpopulation of B cells.
- Published
- 1981
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