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Publication : A tumor-suppressor function for Fas (CD95) revealed in T cell-deficient mice.

First Author  Peng SL Year  1996
Journal  J Exp Med Volume  184
Issue  3 Pages  1149-54
PubMed ID  9064331 Mgi Jnum  J:35237
Mgi Id  MGI:82689 Doi  10.1084/jem.184.3.1149
Citation  Peng SL, et al. (1996) A tumor-suppressor function for Fas (CD95) revealed in T cell-deficient mice. J Exp Med 184(3):1149-54
abstractText  Fas (CD95) and its ligand are central regulatory molecules in hematopoietic cells. Previous studies have suggested a role for Fas in the regulation of tumor progression, but Fas has not yet been conclusively identified as a tumor suppressor. Fas-deficient individuals lack malignant tumors, perhaps because of regulation by T cells. To investigate such a possibility, mice deficient in both T cells and Fas were generated, and they were found to develop severe B cell dysregulation characterized by malignant, lethal B cell lymphoma. Lymphoma arose from a monoclonal B220+CD19-CD5-CD23- B cell secreting immunoglobulin M, kappa rheumatoid factor. In contrast, animals containing alpha beta T cells, gamma delta T cells, and/or functional Fas suppressed the development of lymphoma. These data indicate that Fas functions as a tumor suppressor, and identifies roles for both alpha beta T cells and gamma delta T cells in Fas-independent tumor regulation.
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