Efficacy and Toxicity Management of 19-28z CAR T Cell Therapy in B Cell Acute Lymphoblastic Leukemia

Davila, Marco L.; Rivière, Isabelle; Wang, Xiuyan; Bartido, Shirley; Park, Jae; Curran, Kevin J.; Chung, Stephen S.; Stefanski, Jolanta; Bórquez-Ojeda, Oriana; Olszewska, Malgorzata; Qu, Jinrong; Wasielewska, Teresa; He, Qing; Fink, Mitsú J.; Shinglot, Himaly; Youssif, Maher; Satter, Mark; Wang, Yongzeng; Hosey, James; Quintanilla, Hilda; Halton, Elizabeth; Bernal, Yvette; Bouhassira, Diana; Arcila, Maria E.; Gönen, Mithat; Roboz, Gail J.; Maslak, Peter; Douer, Dan; Frattini, Mark G.; Giralt, Sergío; Sadelain, Michel; Brentjens, Renier J.

doi:10.1126/scitranslmed.3008226

Cited by 2,099 publications

(2,310 citation statements)

References 31 publications

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“…14,20,23–25 Toxicity has been associated with acute, massive cytokine release in some immunotherapeutics, such as CAR T-cells. 49 Cytokines were not monitored in this study as their importance in a tumor-free animal is questionable. In most primates, cellular immunity rapidly contracted after boosting.…”

Section: Discussionmentioning

confidence: 99%

Preclinical evaluation of a MAGE-A3 vaccination utilizing the oncolytic Maraba virus currently in first-in-human trials

et al. 2018

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Multiple immunotherapeutics have been approved for cancer patients, however advanced solid tumors are frequently refractory to treatment. We evaluated the safety and immunogenicity of a vaccination approach with multimodal oncolytic potential in non-human primates (NHP) (Macaca fascicularis). Primates received a replication-deficient adenoviral prime, boosted by the oncolytic Maraba MG1 rhabdovirus. Both vectors expressed the human MAGE-A3. No severe adverse events were observed. Boosting with MG1-MAGEA3 induced an expansion of hMAGE-A3-specific CD4+ and CD8+ T-cells with the latter peaking at remarkable levels and persisting for several months. T-cells reacting against epitopes fully conserved between simian and human MAGE-A3 were identified. Humoral immunity was demonstrated by the detection of circulating MAGE-A3 antibodies. These preclinical data establish the capacity for the Ad:MG1 vaccination to engage multiple effector immune cell populations without causing significant toxicity in outbred NHPs. Clinical investigations utilizing this program for the treatment of MAGE-A3-positive solid malignancies are underway (NCT02285816, NCT02879760).

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Section: Discussionmentioning

confidence: 99%

Preclinical evaluation of a MAGE-A3 vaccination utilizing the oncolytic Maraba virus currently in first-in-human trials

et al. 2018

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“…7 High-dose corticosteroids have been used in patients, although there is some evidence that they may have a detrimental effect on T cell proliferation; therefore, their use is reserved for management of continuing severe CRS and/or severe neurologic toxicity. 10 Predictive biomarkers of which patients are likely to experience CRS are being explored. 11 More extensive reviews of the grading and management of CRS have been published, 7,12 and the algorithms for clinical management are still in development by the various sponsors of CAR T cell therapies.…”

Section: Bystander Innate Cellsmentioning

confidence: 99%

The Flipside of the Power of Engineered T Cells: Observed and Potential Toxicities of Genetically Modified T Cells as Therapy

2017

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“…(Sadelain 2015) Several groups have reported CR rates as high as 90% in ALL after administration of a single dose of CD19-CAR T-cells following lymphodepleting chemotherapy, even in heavily pre-treated children and adults. (Davila et al 2014, Lee et al 2015, Maude et al 2014) The success of CD19-specific T-cells in early phase trials has resulted in the designation of “FDA breakthrough status” and commercialization efforts. (June et al 2015, Sadelain 2015) There are currently 45 actively enrolling clinical trials targeting CD19 with CAR T-cells.…”

Section: Chimeric Antigen Receptor-modified T-cellsmentioning

confidence: 99%

“…(Davila et al 2014, Park et al 2016). Of 45 evaluable patients with morphological relapse or MRD, 37 achieved or maintained morphological CR, with no detectable MRD in 30.…”

Section: Chimeric Antigen Receptor-modified T-cellsmentioning

confidence: 99%

“…(Rooney et al 2014, Sadelain 2015, Vonderheide and June 2014) Indeed, this is an exciting time in the field of T-cell immunotherapy with in vitro discoveries paving the way for bench-to-bedside translation and resulting in remarkable clinical responses in a variety of haematological malignancies. In particular, adoptively transferred T-cells genetically modified to express CD19 CARs have shown great promise (Davila et al 2014, Lee et al 2015, Maude et al 2014), although some haematological malignancies remain recalcitrant. For these tumours, combination immunotherapeutic approaches are being investigated and may prove beneficial.…”

Section: Introductionmentioning

confidence: 99%

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Recent advances in T‐cell immunotherapy for haematological malignancies

et al. 2016

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In vitro discoveries have paved the way for bench-to-bedside translation in adoptive T cell immunotherapy, resulting in remarkable clinical responses in a variety of haematological malignancies. Adoptively transferred T cells genetically modified to express CD19 CARs have shown great promise, although many unanswered questions regarding how to optimize T-cell therapies for both safety and efficacy remain. Similarly, T cells that recognize viral or tumour antigens though their native receptors have produced encouraging clinical responses. Honing manufacturing processes will increase the availability of T-cell products, while combining T-cell therapies has the ability to increase complete response rates. Lastly, innovative mechanisms to control these therapies may improve safety profiles while genome editing offers the prospect of modulating T-cell function. This review will focus on recent advances in T-cell immunotherapy, highlighting both clinical and pre-clinical advances, as well as exploring what the future holds.

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Efficacy and Toxicity Management of 19-28z CAR T Cell Therapy in B Cell Acute Lymphoblastic Leukemia

Cited by 2,099 publications

References 31 publications

Preclinical evaluation of a MAGE-A3 vaccination utilizing the oncolytic Maraba virus currently in first-in-human trials

Preclinical evaluation of a MAGE-A3 vaccination utilizing the oncolytic Maraba virus currently in first-in-human trials

The Flipside of the Power of Engineered T Cells: Observed and Potential Toxicities of Genetically Modified T Cells as Therapy

Recent advances in T‐cell immunotherapy for haematological malignancies

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