Expansion of myeloid suppressor cells in SHIP-deficient mice represses allogeneic T cell responses |
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| Authors: | Ghansah Tomar Paraiso Kim H T Highfill Steven Desponts Caroline May Sarah McIntosh Joseph K Wang Jia-Wang Ninos John Brayer Jason Cheng Fengdong Sotomayor Eduardo Kerr William G |
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| Affiliation: | Immunology Program, H. Lee Moffitt Comprehensive Cancer Center and Research Institute, and Department of Interdisciplinary Oncology, University of South Florida, Tampa, FL 33612, USA. |
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| Abstract: | Previously we demonstrated that SHIP(-/-) mice accept allogeneic bone marrow transplants (BMT) without significant acute graft-vs-host disease (GvHD). In this study we show that SHIP(-/-) splenocytes and lymph node cells are poor stimulators of allogeneic T cell responses that cause GvHD. Intriguingly, SHIP(-/-) splenocytes prime naive T cell responses to peptide epitopes, but, conversely, are partially impaired for priming T cell responses to whole Ag. However, dendritic cells (DC) purified from SHIP(-/-) splenocytes prime T cell responses to allogeneic targets, peptide epitopes, and whole Ag as effectively as SHIP(+/+) DC. These findings point to an extrinsic effect on SHIP(-/-) DC that impairs priming of allogeneic T cell responses. Consistent with this extrinsic effect, we found that a dramatic expansion of myeloid suppressor cells in SHIP(-/-) mice impairs priming of allogeneic T cells. These findings suggest that SHIP expression or its activity could be targeted to selectively compromise T cell responses that mediate GvHD and graft rejection. |
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