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Evidence of long‐lasting anti‐CD19 activity of engrafted CD19 chimeric antigen receptor–modified T cells in a phase I study targeting pediatrics with acute lymphoblastic leukemia

Ninety percent of relapse/refractory B‐cell acute lymphatic leukemia (R/R B‐ALL) patients can achieve complete remission (CR) after CD19‐targeting chimeric antigen receptor T (CAR‐T) cell therapy. However, around 50% of them relapse in 1 year. Persistent CAR‐T cell engraftment is considered as the k...

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Autores principales: Ma, Futian, Ho, Jin‐Yuan, Du, Huan, Xuan, Fan, Wu, Xiaoli, Wang, Qinglong, Wang, Lin, Liu, Ying, Ba, Min, Wang, Yizhuo, Luo, Jianmin, Li, Jianqiang
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2019
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6973049/
https://www.ncbi.nlm.nih.gov/pubmed/31465532
http://dx.doi.org/10.1002/hon.2672
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author Ma, Futian
Ho, Jin‐Yuan
Du, Huan
Xuan, Fan
Wu, Xiaoli
Wang, Qinglong
Wang, Lin
Liu, Ying
Ba, Min
Wang, Yizhuo
Luo, Jianmin
Li, Jianqiang
author_facet Ma, Futian
Ho, Jin‐Yuan
Du, Huan
Xuan, Fan
Wu, Xiaoli
Wang, Qinglong
Wang, Lin
Liu, Ying
Ba, Min
Wang, Yizhuo
Luo, Jianmin
Li, Jianqiang
author_sort Ma, Futian
collection PubMed
description Ninety percent of relapse/refractory B‐cell acute lymphatic leukemia (R/R B‐ALL) patients can achieve complete remission (CR) after CD19‐targeting chimeric antigen receptor T (CAR‐T) cell therapy. However, around 50% of them relapse in 1 year. Persistent CAR‐T cell engraftment is considered as the key to remain durable remission. Here, we initiated a phase I study to treat 10 pediatric B‐ALL patients using a CD19‐targeted second generation CAR with a 4‐1BB intracellular costimulatory domain. All patients received a standard fludarabine and cyclophosphamide (FC) preconditioning regiment, followed by a CAR‐T infusion with a median number of 0.5 (0.3‐1.58) × 10(6) CAR+ T cells/kg. The pretreatment tumor burdens were high with a median bone marrow (BM) blasts percentage of 59.2% (7.31%‐86.2%), excluding one patient only with brain infiltration of leukemia cells (0% BM blasts). The initial CR rate was 80% (n = 8/10). Four patients (40%) experienced serious (grade > 2) cytokine release syndrome (CRS) and three patients (30%) with obvious neurotoxicity. Monthly assessments of CD19+ minimal residual disease (MRD) and CAR‐T engraftment demonstrated the anti‐CD19 activity of long‐term engrafted CAR‐T cell clones in one patient for more than 2 years.
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spelling pubmed-69730492020-01-27 Evidence of long‐lasting anti‐CD19 activity of engrafted CD19 chimeric antigen receptor–modified T cells in a phase I study targeting pediatrics with acute lymphoblastic leukemia Ma, Futian Ho, Jin‐Yuan Du, Huan Xuan, Fan Wu, Xiaoli Wang, Qinglong Wang, Lin Liu, Ying Ba, Min Wang, Yizhuo Luo, Jianmin Li, Jianqiang Hematol Oncol Original Research Articles Ninety percent of relapse/refractory B‐cell acute lymphatic leukemia (R/R B‐ALL) patients can achieve complete remission (CR) after CD19‐targeting chimeric antigen receptor T (CAR‐T) cell therapy. However, around 50% of them relapse in 1 year. Persistent CAR‐T cell engraftment is considered as the key to remain durable remission. Here, we initiated a phase I study to treat 10 pediatric B‐ALL patients using a CD19‐targeted second generation CAR with a 4‐1BB intracellular costimulatory domain. All patients received a standard fludarabine and cyclophosphamide (FC) preconditioning regiment, followed by a CAR‐T infusion with a median number of 0.5 (0.3‐1.58) × 10(6) CAR+ T cells/kg. The pretreatment tumor burdens were high with a median bone marrow (BM) blasts percentage of 59.2% (7.31%‐86.2%), excluding one patient only with brain infiltration of leukemia cells (0% BM blasts). The initial CR rate was 80% (n = 8/10). Four patients (40%) experienced serious (grade > 2) cytokine release syndrome (CRS) and three patients (30%) with obvious neurotoxicity. Monthly assessments of CD19+ minimal residual disease (MRD) and CAR‐T engraftment demonstrated the anti‐CD19 activity of long‐term engrafted CAR‐T cell clones in one patient for more than 2 years. John Wiley and Sons Inc. 2019-09-15 2019-12 /pmc/articles/PMC6973049/ /pubmed/31465532 http://dx.doi.org/10.1002/hon.2672 Text en ©2019 John Wiley & Sons, Ltd. This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Research Articles
Ma, Futian
Ho, Jin‐Yuan
Du, Huan
Xuan, Fan
Wu, Xiaoli
Wang, Qinglong
Wang, Lin
Liu, Ying
Ba, Min
Wang, Yizhuo
Luo, Jianmin
Li, Jianqiang
Evidence of long‐lasting anti‐CD19 activity of engrafted CD19 chimeric antigen receptor–modified T cells in a phase I study targeting pediatrics with acute lymphoblastic leukemia
title Evidence of long‐lasting anti‐CD19 activity of engrafted CD19 chimeric antigen receptor–modified T cells in a phase I study targeting pediatrics with acute lymphoblastic leukemia
title_full Evidence of long‐lasting anti‐CD19 activity of engrafted CD19 chimeric antigen receptor–modified T cells in a phase I study targeting pediatrics with acute lymphoblastic leukemia
title_fullStr Evidence of long‐lasting anti‐CD19 activity of engrafted CD19 chimeric antigen receptor–modified T cells in a phase I study targeting pediatrics with acute lymphoblastic leukemia
title_full_unstemmed Evidence of long‐lasting anti‐CD19 activity of engrafted CD19 chimeric antigen receptor–modified T cells in a phase I study targeting pediatrics with acute lymphoblastic leukemia
title_short Evidence of long‐lasting anti‐CD19 activity of engrafted CD19 chimeric antigen receptor–modified T cells in a phase I study targeting pediatrics with acute lymphoblastic leukemia
title_sort evidence of long‐lasting anti‐cd19 activity of engrafted cd19 chimeric antigen receptor–modified t cells in a phase i study targeting pediatrics with acute lymphoblastic leukemia
topic Original Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6973049/
https://www.ncbi.nlm.nih.gov/pubmed/31465532
http://dx.doi.org/10.1002/hon.2672
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