1999
DOI: 10.1007/978-1-4615-4987-1_6
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Allogeneic Hematopoietic Stem Cell Transplantation in Recipients of Cellular or Solid Organ Allografts

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Cited by 2 publications
(3 citation statements)
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“…Alternatively, their MLR-suppressing activity and Th2-like IL-4 production may contribute to protecting developing B cells from potentially autoreactive Th1 cells in the BM microenvironment. In either case, these results, in conjunction with previous murine and human data (13,(21)(22)(23)(24)(25)(26)(27)(28)(29)(30)(31), indicate that BM-derived CD1d-reactive T cells may regulate GvHD in allogeneic BM transplantation and contribute to allograft tolerance. Therapeutic expansion of such cells in the setting of hemopoietic cell transplantation may provide a means to suppress GvHD, which complements the potential graft-vs-tumor activity of other NK T cells (15,16,33,36).…”
Section: Cd1d-reactive Bm-derived T Cells Specifically Suppress Mlrsupporting
confidence: 75%
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“…Alternatively, their MLR-suppressing activity and Th2-like IL-4 production may contribute to protecting developing B cells from potentially autoreactive Th1 cells in the BM microenvironment. In either case, these results, in conjunction with previous murine and human data (13,(21)(22)(23)(24)(25)(26)(27)(28)(29)(30)(31), indicate that BM-derived CD1d-reactive T cells may regulate GvHD in allogeneic BM transplantation and contribute to allograft tolerance. Therapeutic expansion of such cells in the setting of hemopoietic cell transplantation may provide a means to suppress GvHD, which complements the potential graft-vs-tumor activity of other NK T cells (15,16,33,36).…”
Section: Cd1d-reactive Bm-derived T Cells Specifically Suppress Mlrsupporting
confidence: 75%
“…Human BM similarly contains cells that can suppress MLR (25,26) and GvHD and induce tolerance to allografts (27)(28)(29)(30)(31). We report in this work that human BM was highly enriched for CD161 ϩ noninvariant CD1d-reactive T cells.…”
mentioning
confidence: 75%
“…In this group, we examined the effect of intraportal codelivery of islets and DBMCs on POD 0, followed by intravenous infusions of DBMCs on PODs 4 or 5 and 11. The timing of DBMC infusion was based on previous clinical studies, in which delayed marrow infusion was found to be optimal in the setting of solid organ or islet transplantation (35). Group 2 had eight animals that received the same induction therapy with thymoglobulin and fludarabine.…”
Section: Methodsmentioning
confidence: 99%