Persistence and Efficacy of Second Generation CAR T Cell Against the LeY Antigen in Acute Myeloid Leukemia

David S. Ritchie; Paul J. Neeson; Amit Khot; Stefan Peinert; Tsin Yee Tai; Kellie M. Tainton; Karen Chen; Mandy Shin; Dominic Wall; Dirk Hönemann; Peter Gambell; David Westerman; Javier Haurat; Jennifer A. Westwood; Andrew M. Scott; L. Ya. Kravets; Michael Dickinson; Joseph A. Trapani; Mark J. Smyth; Phillip K. Darcy; Michael H. Kershaw; H. Miles Prince

doi:10.1038/mt.2013.154

Persistence and Efficacy of Second Generation CAR T Cell Against the LeY Antigen in Acute Myeloid Leukemia

David S. Ritchie(The University of Melbourne), Paul J. Neeson(The University of Melbourne), Amit Khot(Peter MacCallum Cancer Centre), Stefan Peinert(Peter MacCallum Cancer Centre), Tsin Yee Tai(Peter MacCallum Cancer Centre), Kellie M. Tainton(Peter MacCallum Cancer Centre), Karen Chen(Peter MacCallum Cancer Centre), Mandy Shin(Peter MacCallum Cancer Centre), Dominic Wall(Peter MacCallum Cancer Centre), Dirk Hönemann(Peter MacCallum Cancer Centre), Peter Gambell(Peter MacCallum Cancer Centre), David Westerman(Peter MacCallum Cancer Centre), Javier Haurat(Peter MacCallum Cancer Centre), Jennifer A. Westwood(The University of Melbourne), Andrew M. Scott(Ludwig Cancer Research), L. Ya. Kravets(Peter MacCallum Cancer Centre), Michael Dickinson(Peter MacCallum Cancer Centre), Joseph A. Trapani(The University of Melbourne), Mark J. Smyth(The University of Melbourne), Phillip K. Darcy(The University of Melbourne), Michael H. Kershaw(The University of Melbourne), H. Miles Prince(The University of Melbourne)

Molecular Therapy

July 8, 2013

10.1038/mt.2013.154

Cited by 431Open Access

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Abstract

In a phase I study of autologous chimeric antigen receptor (CAR) anti-LeY T-cell therapy of acute myeloid leukemia (AML), we examined the safety and postinfusion persistence of adoptively transferred T cells. Following fludarabine-containing preconditioning, four patients received up to 1.3 × 109 total T cells, of which 14–38% expressed the CAR. Grade 3 or 4 toxicity was not observed. One patient achieved a cytogenetic remission whereas another with active leukemia had a reduction in peripheral blood (PB) blasts and a third showed a protracted remission. Using an aliquot of In111-labeled CAR T cells, we demonstrated trafficking to the bone marrow (BM) in those patients with the greatest clinical benefit. Furthermore, in a patient with leukemia cutis, CAR T cells infiltrated proven sites of disease. Serial PCR of PB and BM for the LeY transgene demonstrated that infused CAR T cells persisted for up to 10 months. Our study supports the feasibility and safety of CAR–T-cell therapy in high-risk AML, and demonstrates durable in vivo persistence. In a phase I study of autologous chimeric antigen receptor (CAR) anti-LeY T-cell therapy of acute myeloid leukemia (AML), we examined the safety and postinfusion persistence of adoptively transferred T cells. Following fludarabine-containing preconditioning, four patients received up to 1.3 × 109 total T cells, of which 14–38% expressed the CAR. Grade 3 or 4 toxicity was not observed. One patient achieved a cytogenetic remission whereas another with active leukemia had a reduction in peripheral blood (PB) blasts and a third showed a protracted remission. Using an aliquot of In111-labeled CAR T cells, we demonstrated trafficking to the bone marrow (BM) in those patients with the greatest clinical benefit. Furthermore, in a patient with leukemia cutis, CAR T cells infiltrated proven sites of disease. Serial PCR of PB and BM for the LeY transgene demonstrated that infused CAR T cells persisted for up to 10 months. Our study supports the feasibility and safety of CAR–T-cell therapy in high-risk AML, and demonstrates durable in vivo persistence.

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