Next Generation Veto Cells for Non-Myeloablative Haploidentical HSCT: Combining Anti-Viral and Graft Facilitating Activity

Abstract: Transplantation of T cell-depleted BM (TDBM) under mild conditioning, associated with minimal toxicity and reduced risk of GVHD, offers an attractive therapeutic option for patients with nonmalignant hematologic disorders or can be used to induce immune tolerance to subsequent organ transplantation. However, overcoming TDBM rejection after reduced conditioning remains a challenge. We previously demonstrated that this barrier can be overcome using donor-derived naïve CD8 T cells if they are expanded against thi… Show more

“…Results showed that Tcm grown from a starting population of CD8 + CD44 + cells were also able to achieve marked donor chimerism when administered with megadose TCD allogeneic HSCT in sublethally irradiated Balb/c recipients. Notably, infusion of 5 × 10 6 Tcm into sublethally irradiated mice (5.5 Gy TBI) without BMT did not cause any GVHD, as measured by weight loss, in contrast to the CD8 + CD44 + T cells used to generate the Tcm [43].…”

“…The resulting population was subjected to third-party stimulation by coculture with irradiated splenocytes generated from spleens of OVA-expressing mice under cytokine deprivation. HIL-15 (10 ng/mL) was added to the culture at 60 hours after culture initiation to induce the cells to express a Tcm-like phenotype, as described previously for anti-third-party Tcm generated from WT naïve CD8 + T cells (WT Tcm) [43].…”

“…When tested in vivo, the OT-1 Tcm (H2Kb) were able to enhance engraftment after allogeneic T cell-depleted BMT (H2b) in sublethally irradiated (5.5 Gy TBI) Balb/c recipients (H2Kd), in analogy to the chimerism induced by WT Tcm [43]. This initial successful experiment was then followed by an experiment, which more closely resembled the human setting, in which the CD8 + CD44 + cells were isolated from WT C57BL/6 OVA-immunized mice and subsequently introduced to coculture with irradiated splenocytes generated from spleens of OVA-expressing mice.…”

“…Dr Reisner concluded that potent veto CD8 + Tcm can be generated from the memory pool of donors positive for viral reactivity by stimulation against viral antigens. Such veto Tcm could be most attractive for T cell-depleted BM HaploSCT, because they can enable engraftment following NMA conditioning while at the same time providing antiviral protection [43].…”

Proceedings From the Fourth Haploidentical Stem Cell Transplantation Symposium (HAPLO2016), San Diego, California, December 1, 2016

“…Results showed that Tcm grown from a starting population of CD8 + CD44 + cells were also able to achieve marked donor chimerism when administered with megadose TCD allogeneic HSCT in sublethally irradiated Balb/c recipients. Notably, infusion of 5 × 10 6 Tcm into sublethally irradiated mice (5.5 Gy TBI) without BMT did not cause any GVHD, as measured by weight loss, in contrast to the CD8 + CD44 + T cells used to generate the Tcm [43].…”

“…The resulting population was subjected to third-party stimulation by coculture with irradiated splenocytes generated from spleens of OVA-expressing mice under cytokine deprivation. HIL-15 (10 ng/mL) was added to the culture at 60 hours after culture initiation to induce the cells to express a Tcm-like phenotype, as described previously for anti-third-party Tcm generated from WT naïve CD8 + T cells (WT Tcm) [43].…”

“…When tested in vivo, the OT-1 Tcm (H2Kb) were able to enhance engraftment after allogeneic T cell-depleted BMT (H2b) in sublethally irradiated (5.5 Gy TBI) Balb/c recipients (H2Kd), in analogy to the chimerism induced by WT Tcm [43]. This initial successful experiment was then followed by an experiment, which more closely resembled the human setting, in which the CD8 + CD44 + cells were isolated from WT C57BL/6 OVA-immunized mice and subsequently introduced to coculture with irradiated splenocytes generated from spleens of OVA-expressing mice.…”

“…Dr Reisner concluded that potent veto CD8 + Tcm can be generated from the memory pool of donors positive for viral reactivity by stimulation against viral antigens. Such veto Tcm could be most attractive for T cell-depleted BM HaploSCT, because they can enable engraftment following NMA conditioning while at the same time providing antiviral protection [43].…”

Proceedings From the Fourth Haploidentical Stem Cell Transplantation Symposium (HAPLO2016), San Diego, California, December 1, 2016

Towards ‘off-the-shelf’ genetically modified T cells: prolonging functional engraftment in mice by CD8 veto T cells

Next-generation CD8 memory veto T cells directed against memory antigens