Durable Responses and Low Toxicity After Fast Off-Rate CD19 Chimeric Antigen Receptor-T Therapy in Adults With Relapsed or Refractory B-Cell Acute Lymphoblastic Leukemia

Claire Roddie(CRUK Lung Cancer Centre of Excellence), Juliana Dias(Royal Free London NHS Foundation Trust), Maeve O’Reilly, Mahnaz Abbasian(University College London), Amaia Cadiñanos-Garai(University College London), Ketki Vispute(University College London), Leticia Bosshard‐Carter(University College London), Marina Mitsikakou(University College London), Vedika Mehra(University College London), Harriet Roddy(University College London), John A. Hartley(University College London), Victoria J. Spanswick(University College London), Helen L. Lowe(University College London), Bilyana Popova(CRUK Lung Cancer Centre of Excellence), Laura Clifton‐Hadley(CRUK Lung Cancer Centre of Excellence), Graham Wheeler(CRUK Lung Cancer Centre of Excellence), Joanna Olejnik(CRUK Lung Cancer Centre of Excellence), Adrian Bloor(The Christie Hospital), David Irvine(Queen Elizabeth University Hospital), L. Wood, Maria A. V. Marzolini, Sabine Domning(King's College London), Farzin Farzaneh(King's College London), Mark W. Lowdell(Royal Free London NHS Foundation Trust), David C. Linch(University College London), Martin Pulé(Autolus (United Kingdom)), Karl S. Peggs(CRUK Lung Cancer Centre of Excellence)
Journal of Clinical Oncology
August 31, 2021
10.1200/jco.21.00917
Cited by 139Open Access
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Abstract

PURPOSE: Prognosis for adult B-cell acute lymphoblastic leukemia (B-ALL) is poor, and there are currently no licensed CD19 chimeric antigen receptor (CAR) therapeutics. We developed a novel second-generation CD19-CAR (CAT19-41BB-Z) with a fast off rate, designed for more physiologic T-cell activation to reduce toxicity and improve engraftment. We describe the multicenter phase I ALLCAR19 (NCT02935257) study of autologous CAT19-41BB-Z CAR T cells (AUTO1) in relapsed or refractory (r/r) adult B-ALL. METHODS: Patients age ≥ 16 years with r/r B-ALL were eligible. Primary outcomes were toxicity and manufacturing feasibility. Secondary outcomes were depth of response at 1 and 3 months, persistence of CAR-T, incidence and duration of hypogammaglobulinemia and B-cell aplasia, and event-free survival and overall survival at 1 and 2 years. RESULTS: Twenty-five patients were leukapheresed, 24 products were manufactured, and 20 patients were infused with AUTO1. The median age was 41.5 years; 25% had prior blinatumomab, 50% prior inotuzumab ozogamicin, and 65% prior allogeneic stem-cell transplantation. At the time of preconditioning, 45% had ≥ 50% bone marrow blasts. No patients experienced ≥ grade 3 cytokine release syndrome; 3 of 20 (15%) experienced grade 3 neurotoxicity that resolved to ≤ grade 1 within 72 hours with steroids. Seventeen of 20 (85%) achieved minimal residual disease-negative complete response at month 1, and 3 of 17 underwent allogeneic stem-cell transplantation while in remission. The event-free survival at 6 and 12 months was 68.3% (42.4%-84.4%) and 48.3% (23.1%-69.7%), respectively. High-level expansion (Cmax 127,152 copies/µg genomic DNA) and durable CAR-T persistence were observed with B-cell aplasia ongoing in 15 of 20 patients at last follow-up. CONCLUSION: AUTO1 demonstrates a tolerable safety profile, high remission rates, and excellent persistence in r/r adult B-ALL. Preliminary data support further development of AUTO1 as a stand-alone treatment for r/r adult B-ALL.

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