Journal
TRENDS IN IMMUNOLOGY
Volume 42, Issue 3, Pages 261-272Publisher
CELL PRESS
DOI: 10.1016/j.it.2021.01.004
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Funding
- National Cancer Institute [F99CA253757, P50CA126752, P01CA094237]
- Meg Vosburg T Cell Lymphoma Dream Team [SU2C/AACR 604817]
- Leukemia and Lymphoma Society
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Banked allogeneic or 'off-the-shelf' (OTS) T cells from healthy human donors are being developed to address the limitations of autologous cell therapies. Potential challenges of OTS T cell therapies are associated with their allogeneic origin and the possibility of graft-versus-host disease (GvHD) and host-versus-graft immune reactions. While approaches to prevent immune rejection of OTS cells are at an earlier stage of development, the risk of GvHD from OTS T cells has been proved to be manageable in clinical studies.
Banked allogeneic or 'off-the-shelf' (OTS) T cells from healthy human donors are being developed to address the limitations of autologous cell therapies. Potential challenges of OTS T cell therapies are associated with their allogeneic origin and the possibility of graft-versus-host disease (GvHD) and host-versus-graft immune reactions. While the risk of GvHD from OTS T cells has been proved to be manageable in clinical studies, approaches to prevent immune rejection of OTS cells are at an earlier stage of development. We provide an overview of strategies to generate OTS cell therapies and mitigate alloreactivity-associated adverse events, with a focus on recent advances for preventing immune rejection.
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