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Publication : Veto activity of activated bone marrow does not require perforin and Fas ligand.

First Author  Chrobak P Year  2001
Journal  Cell Immunol Volume  208
Issue  2 Pages  80-7
PubMed ID  11333140 Mgi Jnum  J:127838
Mgi Id  MGI:3765129 Doi  10.1006/cimm.2001.1771
Citation  Chrobak P, et al. (2001) Veto activity of activated bone marrow does not require perforin and Fas ligand. Cell Immunol 208(2):80-7
abstractText  Veto cells suppress generation of CD8(+) T cell immune responses in an antigen-specific manner, with specificity dictated by antigens on the veto cell surface. Activated bone marrow (ABM) veto cells belong to the NK cell type lineage and veto by clonally deleting antigen-specific precursor cytotoxic T cell lymphocyte (CTL). In vitro cytotoxicity of ABM depends largely on the perforin/granzyme and Fas/Fas ligand pathways. Utilizing perforin-deficient and functional Fas ligand-deficient gld mice as a source of ABM and functional Fas-deficient lpr mice as a source of precursor CTL, we demonstrate in this study that ABM cells utilize a perforin- and Fas-independent pathway to veto allogeneic cell-mediated cytotoxic responses. We also show that ABM cells mediate perforin- and Fas-independent veto activity even in an 8-h clonal deletion assay. We conclude that ABM veto activity does not require the two primary pathways of cell-mediated death.
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