Literature DB >> 21878902

Combining mTor inhibitors with rapamycin-resistant T cells: a two-pronged approach to tumor elimination.

Leslie E Huye1, Yozo Nakazawa, Mayuri P Patel, Eric Yvon, Jiali Sun, Barbara Savoldo, Matthew H Wilson, Gianpietro Dotti, Cliona M Rooney.   

Abstract

Despite activity as single agent cancer therapies, Rapamycin (rapa) and its rapalogs may have their greatest effects when combined with other therapeutic modalities. In addition to direct antitumor activity, rapalogs reverse multiple tumor-intrinsic immune evasion mechanisms. These should facilitate tumor-specific T cell activity, but since rapa directly inhibits effector T cells, this potential immune enhancement is lost. We hypothesized that if T cells were rendered resistant to rapa they could capitalize on its downregulation of tumor immune evasion. We therefore modified T cells with a rapa-resistant mutant of mTor, mTorRR, and directed them to B lymphomas by coexpressing a chimeric antigen receptor (CAR) for CD19 (CAR.CD19-28ζ). T cells expressing transgenic mTorRR from a piggyBac transposon maintain mTor signaling, proliferate in the presence of rapa and retain their cytotoxic function and ability to secrete interferon-γ (IFNγ) after stimulation, effector functions that were inhibited by rapa in control T cells. In combination, rapa and rapa-resistant-CAR.CD19-28ζ-expressing T cells produced greater antitumor activity against Burkitt's lymphoma and pre-B ALL cell lines in vitro than CAR.CD19-28ζ T cells or rapa alone. In conclusion, the combination of rapa and rapa-resistant, CAR.CD19-28ζ-expressing T cells may provide a novel therapy for the treatment of B cell malignancies and other cancers.

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Year:  2011        PMID: 21878902      PMCID: PMC3242659          DOI: 10.1038/mt.2011.179

Source DB:  PubMed          Journal:  Mol Ther        ISSN: 1525-0016            Impact factor:   11.454


  37 in total

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2.  Optimization of the PiggyBac transposon system for the sustained genetic modification of human T lymphocytes.

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10.  T cells expressing constitutively active Akt resist multiple tumor-associated inhibitory mechanisms.

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  24 in total

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Review 7.  CAR T-cell therapy of solid tumors.

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Review 8.  Design and implementation of adoptive therapy with chimeric antigen receptor-modified T cells.

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Review 9.  Rapamycin-resistant effector T-cell therapy.

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10.  Engineering T cells for cancer: our synthetic future.

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