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Early regulation of CD8 T cell alloreactivity by CD4<sup>+</sup>CD25<sup>– </sup>T cells in recipients of anti‐CD154 antibody and allogeneic BMT is followed by rapid peripheral deletion of donor‐reactive CD8<sup>+</sup> T cells, precluding a role for sustained regulation
74
Citations
48
References
2005
Year
Adaptive Immune SystemT-regulatory CellImmunologyImmune RegulationImmunodominanceCd4+cd25- T CellsCd4 T Cell ResponsesMixed ChimerismImmunotherapySustained RegulationCell TransplantationCell SignalingRegulatory T Cell BiologyEarly RegulationAllergyAutoimmune DiseaseRapid Peripheral DeletionAutoimmunityHumoral ImmunityT Cell ImmunityTolerance InductionCell BiologyT Cell BiologyCellular Immune ResponseMedicineCd8 Cell Tolerance
While acquisition of regulatory function by CD4+CD25- T cells has been reported following antigenic stimulation, "naturally occurring" regulatory CD4+ T cells (Treg) are believed to express CD25. We examined the mechanisms involved in peripheral CD8 T cell tolerance by induction of mixed chimerism using non-myeloablative conditioning with low-dose (3 Gy) total body irradiation and anti-CD154 antibody. Recipient CD4+ T cells were initially required for the induction of CD8 cell tolerance, but were not needed beyond 2 weeks. Depletion of CD25+ Treg prior to bone marrow transplantation and blockade of IL-2 with neutralizing antibody did not impede tolerance induction. Tolerance was dependent on CTLA4, but not on IFN-gamma. In C57BL/6 mice containing a fraction of 2C TCR transgenic CD8+ T cells, which recognize the MHC class I alloantigen Ld, induction of chimerism with L(d+), but not Ld-, bone marrow cells led to deletion of peripheral 2C+ CD8+ cells within 1 week in peripheral blood and spleen. Complete deletion required the presence of recipient CD4+ T cells. Thus, a novel, rapid form of regulation by CD4+CD25- T cells permits initial CD8 T cell tolerance in this model. Rapid peripheral deletion of donor-specific CD8 T cells precludes an ongoing requirement for CD4 T cell-mediated regulation.
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