| Literature DB >> 27872095 |
Teresa Manzo1,2, Tabea Sturmheit1,2, Veronica Basso1, Elisabetta Petrozziello1,2, Rodrigo Hess Michelini1, Michela Riba3, Massimo Freschi4, Angela R Elia1, Matteo Grioni1, Flavio Curnis5, Maria Pia Protti1, Ton N Schumacher6, Reno Debets7, Melody A Swartz8,9, Angelo Corti2,5, Matteo Bellone1, Anna Mondino10.
Abstract
Donor-derived allogeneic T cells evoke potent graft versus tumor (GVT) effects likely due to the simultaneous recognition of tumor-specific and host-restricted minor histocompatibility (H) antigens. Here we investigated whether such effects could be reproduced in autologous settings by TCR gene-engineered lymphocytes. We report that T cells redirected either to a broadly expressed Y-encoded minor H antigen or to a tumor-associated antigen, although poorly effective if individually transferred, when simultaneously administered enabled acute autochthonous tumor debulking and resulted in durable clinical remission. Y-redirected T cells proved hyporesponsive in peripheral lymphoid organs, whereas they retained effector function at the tumor site, where in synergy with tumor-redirected lymphocytes, they instructed TNFα expression, endothelial cell activation, and intratumoral T-cell infiltration. While neutralizing TNFα hindered GVT effects by the combined T-cell infusion, a single injection of picogram amounts of NGR-TNF, a tumor vessel-targeted TNFα derivative currently in phase III clinical trials, substituted for Y-redirected cells and enabled tumor debulking by tumor-redirected lymphocytes. Together, our results provide new mechanistic insights into allogeneic GVT, validate the importance of targeting the tumor and its associated stroma, and prove the potency of a novel combined approach suitable for immediate clinical implementation. Cancer Res; 77(3); 658-71. ©2016 AACR. ©2016 American Association for Cancer Research.Entities:
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Year: 2016 PMID: 27872095 DOI: 10.1158/0008-5472.CAN-16-0725
Source DB: PubMed Journal: Cancer Res ISSN: 0008-5472 Impact factor: 12.701