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Phase 1 clinical trial of CRISPR-engineered CAR19 universal T cells for treatment of children with refractory B cell leukemia

阿勒姆图祖马 氟达拉滨 免疫学 CD52型 生物 医学 细胞因子释放综合征 嵌合抗原受体 T细胞 环磷酰胺 内科学 免疫系统 抗体 化疗
作者
Giorgio Ottaviano,Christos Georgiadis,Soragia Athina Gkazi,Farhatullah Syed,Hong Zhan,Annie Etuk,Roland Preece,Jan Chu,Agnieszka Kubat,Stuart Adams,Paul Veys,Ajay Vora,Kanchan Rao,Waseem Qasim,Jesmina James,Kimberly Gilmour,Sarah Inglott,Rebecca Thomas,Lana Mhaldien,Attia Hasnain,Natalia Izotova,Nina Tailor,Barry Flutter,Batoul Ahmed,Toni Braybrook,Danielle Pinner,Lindsey Williams,Ka-Yuk Ko,Anna Taylor,Adebimpe Eshilokun,S Staddon,Persis Amrolia,Robert Chiesa,Giovanna Lucchini,Arina Lazareva,Khushnuma Mullanfiroze,Annette Hill,Maria Finch,Rachel Mead,Lindsey Young,Chris Abbott,Philip Ancliff,Sara Ghorashian,Sujith Samarasinghe,Anupama Rao,Jack Bartram,Vesna Pavasovic,Danny Cheng,Ayad Eddaoudi,Farzin Farzaneh,Sabine Domning,Rene Heimke,Richard Gabriel,Martin G. Sauer,Rita Beier,Kirste Madeleine,Cornelia Eckert,Marco W. Schilham,Anja M. Jansen-Hoogendijk,Jin‐Soo Kim,Daesik Kim
出处
期刊:Science Translational Medicine [American Association for the Advancement of Science (AAAS)]
卷期号:14 (668) 被引量:84
标识
DOI:10.1126/scitranslmed.abq3010
摘要

Genome editing of allogeneic T cells can provide “off-the-shelf” alternatives to autologous chimeric antigen receptor (CAR) T cell therapies. Disruption of T cell receptor α chain (TRAC) to prevent graft-versus-host disease (GVHD) and removal of CD52 (cluster of differentiation 52) for a survival advantage in the presence of alemtuzumab have previously been investigated using transcription activator–like effector nuclease (TALEN)-mediated knockout. Here, we deployed next-generation CRISPR-Cas9 editing and linked CAR expression to multiplexed DNA editing of TRAC and CD52 through incorporation of self-duplicating CRISPR guide RNA expression cassettes within the 3’ long terminal repeat of a CAR19 lentiviral vector. Three cell banks of TT52CAR19 T cells were generated and cryopreserved. A phase 1, open-label, non-randomized clinical trial was conducted and treated six children with relapsed/refractory CD19-positive B cell acute lymphoblastic leukemia (B-ALL) (NCT04557436). Lymphodepletion included fludarabine, cyclophosphamide, and alemtuzumab and was followed by a single infusion of 0.8 × 10 6 to 2.0 × 10 6 CAR19 T cells per kilogram with no immediate toxicities. Four of six patients infused with TT52CAR19 T cells exhibited cell expansion, achieved flow cytometric remission, and then proceeded to receive allogeneic stem cell transplantation. Two patients required biological intervention for grade II cytokine release syndrome, one patient developed transient grade IV neurotoxicity, and one patient developed skin GVHD, which resolved after transplant conditioning. Other complications were within expectations, and primary safety objectives were met. This study provides a demonstration of the feasibility, safety, and therapeutic potential of CRISPR-engineered immunotherapy.
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