[HTML][HTML] A chimeric T cell antigen receptor that augments cytokine release and supports clonal expansion of primary human T cells

MA Pulè, KC Straathof, G Dotti, HE Heslop… - Molecular Therapy, 2005 - cell.com
Molecular Therapy, 2005cell.com
The transduction of primary T cells to express chimeric T cell receptors (cTCR) for redirected
targeting of tumor cells is an attractive strategy for generating tumor-specific T cells for
adoptive therapy. However, tumor cells rarely provide costimulatory signals and hence
cTCRs that transmit just a CD3ζ signal can only initiate target cell killing and interferon-γ
release and fail to induce full activation. Although incorporation of a CD28 component
results in IL-2 release and limited proliferation, T cell activation remains incomplete. OX40 …
Abstract
The transduction of primary T cells to express chimeric T cell receptors (cTCR) for redirected targeting of tumor cells is an attractive strategy for generating tumor-specific T cells for adoptive therapy. However, tumor cells rarely provide costimulatory signals and hence cTCRs that transmit just a CD3ζ signal can only initiate target cell killing and interferon-γ release and fail to induce full activation. Although incorporation of a CD28 component results in IL-2 release and limited proliferation, T cell activation remains incomplete. OX40 transmits a potent and prolonged T cell activation signal and is crucial for maintaining an immunological response. We hypothesize that the CD28-OX40-CD3ζ tripartite cytoplasmic domain will provide a full complement of activation, proliferation, and survival signals for enhanced anti-tumor activity.
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