xid mice reveal the interplay of homeostasis and Bruton's tyrosine kinase-mediated selection at multiple stages of B cell development
Authors
Cancro, Michael P.Sah, Alex P.
Levy, Sherri L.
Allman, David M.
Schmidt, Madelyn R.
Woodland, Robert T.
UMass Chan Affiliations
Department of PhysiologyDepartment of Molecular Genetics and Microbiology
Graduate School of Biomedical Sciences
Document Type
Journal ArticlePublication Date
2001-11-22Keywords
Animals; B-Lymphocyte Subsets; Bone Marrow Cells; Cell Cycle; Cell Differentiation; Cell Lineage; Female; Flow Cytometry; Gene Expression Regulation; Homeostasis; Humans; Immunologic Deficiency; Syndromes; Lymphocyte Count; Male; Mice; Mice, Inbred CBA; Mice, Transgenic; Protein-Tyrosine Kinases; Proto-Oncogene Proteins c-bcl-2; Spleen; Transgenes; X ChromosomeLife Sciences
Medicine and Health Sciences
Metadata
Show full item recordAbstract
Human X-linked agammaglobulinemia (XLA) and murine X-linked immune defect (XID) are both immunodeficiencies mediated by mutations in Bruton's tyrosine kinase (Btk), yet the developmental stage(s) affected remain controversial. To further refine the placement of the XID defect(s), we used bromodeoxyuridine labeling to determine turnover, production and transition rates of developing B cell subsets in normal, xid and xid mice expressing a human Bcl-2 transgene (xid/bcl-2). We find the xid mutation manifest at two stages of B cell development. The first is early, reducing pre-B cell production by restricting pro-B to pre-B cell transit. Surprisingly, this impairment is offset by increased survival of cells progressing from the pre- to immature B cell pool, suggesting that Btk-independent homeostatic mechanisms act to maintain this compartment. The second point of action is late, substantially reducing mature B cell production. Together, these findings reconcile apparent discrepancies in the developmental stage affected by the murine versus human lesions and suggest previously unappreciated homeostatic processes that act at the pre-B to immature B cell transition. Finally, Btk likely functions differently at these two checkpoints, since ectopic Bcl-2 expression fails to directly complement the early xid lesion, yet reverses the defect impeding final B cell maturation.Source
Int Immunol. 2001 Dec;13(12):1501-14.
DOI
10.1093/intimm/13.12.1501Permanent Link to this Item
http://hdl.handle.net/20.500.14038/33278PubMed ID
11717191Related Resources
ae974a485f413a2113503eed53cd6c53
10.1093/intimm/13.12.1501