Kte-C19 (anti-CD19 CAR T Cells) Induces Complete Remissions in Patients with Refractory Diffuse Large B-Cell Lymphoma (DLBCL): Results from the Pivotal Phase 2 Zuma-1

Neelapu, Sattva S.; Locke, Frederick L.; Bartlett, Nancy L.; Lekakis, Lazaros J.; Miklos, David B.; Jacobson, Caron A.; Braunschweig, Ira; Oluwole, Olalekan O.; Siddiqi, Tanya; Lin, Yi; Timmerman, John M.; Stiff, Patrick J.; Friedberg, Jonathan W.; Flinn, Ian W.; Goy, André; Smith, Mitchell R.; Deol, Abhinav; Farooq, Umar; McSweeney, Peter A.; Muñoz, Javier; Avivi, Irit; Castro, Januario E.; Westin, Jason R.; Chávez, Julio C.; Ghobadi, Armin; Komanduri, Krishna V.; Levy, Ronald; Jacobsen, Eric; Reagan, Patrick M.; Bot, Adrian; Rossi, John M.; Navale, Lynn; Jiang, Yizhou; Aycock, Jeff; Elias, Meg; Wiezorek, Jeff; Go, William Y.

doi:10.1182/blood.v128.22.lba-6.lba-6

Cited by 39 publications

(49 citation statements)

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“…Higher serum levels of IL-15, IL-6, IL-10, and IP-10 have been described in patients who develop highgrade neurotoxicity. 126 Second, trafficking of CAR-T cells into the CNS may lead to the development of neurotoxicity. For example, a phase 1 study that included 21 children or young adults with hematologic malignancies who were treated with CD19 CAR-T reported higher concentrations of cerebrospinal fluid CAR-T cells in patients who developed neurotoxicity compared with those who did not.…”

Section: Immune Effector Cell-associated Neurotoxicity Syndromementioning

confidence: 99%

A review of cancer immunotherapy toxicity

Kennedy

Salama

2020

CA A Cancer J Clinicians

930

699

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Cancer immunotherapies, including checkpoint inhibitors and adoptive cell therapy, manipulate the immune system to recognize and attack cancer cells. These therapies have the potential to induce durable responses in multiple solid and hematologic malignancies and thus have transformed treatment algorithms for numerous tumor types. Cancer immunotherapies lead to unique toxicity profiles distinct from the toxicities of other cancer therapies, depending on their mechanism of action. These toxicities often require specific management, which can include steroids and immune‐modulating therapy and for which consensus guidelines have been published. This review will focus on the toxicities of checkpoint inhibitors and chimeric antigen receptor T cells, including pathophysiology, diagnosis, and management.

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Section: Immune Effector Cell-associated Neurotoxicity Syndromementioning

confidence: 99%

A review of cancer immunotherapy toxicity

Kennedy

Salama

2020

CA A Cancer J Clinicians

930

699

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“…The early results of a phase II portion of ZUMA-1 were presented in the late-breaking abstract session of ASH-2016. (34) In total, 101 patients received KTE-C19, and 51 were eligible for analysis at the time. KTE-C19 was successfully manufactured for 99% of the patients enrolled.…”

Section: An Outline Of Car-t Therapymentioning

confidence: 99%

“…Actually, the KTE-C19 phase II trial involved a rapid manufacturing method (designed by the NCI group) and achieved short turnaround time with a low production failure rate. (34,35) Generally, opentissue culture vessels are utilized for CAR-T production, and human serum is required for the cell processing. However, such a complex "open" system takes long time and is difficult to further scale up.…”

Section: Unsolved Problems In Car-t Therapymentioning

confidence: 99%

“…• Early intervention based on cytokine parameters (34,39) • Risk adapted cell dose modification • Incorporation of "suicide gene" or "elimination gene" into CAR-T cell (54,55) • Combination use of ibrutinib (50) 2016. (42) Juno Therapeutics is also studying fully human CD19-CAR-T, JCAR021.…”

Section: ) Cd19 Negative Conversionmentioning

confidence: 99%

“…As described above, some cytokine parameters may help to identify patients at a high risk of CRS; early intervention strategies based on these parameters are a promising approach. (34,39) To reduce the risk of CRS, combined use of Bruton's tyrosine kinase inhibitor, ibrutinib, is a novel and promising strategy. The investigators at UPenn have developed a xenograft model of CRS and compared the cytokine levels and survival after infusion of CAR-T alone or CAR-T in combination with ibrutinib.…”

Section: ) Cd19 Negative Conversionmentioning

confidence: 99%

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Clinical development of anti‐CD19 chimeric antigen receptor T‐cell therapy for B‐cell non‐Hodgkin lymphoma

Makita

Yoshimura²,

Tobinai

2017

Cancer Science

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B‐cell non‐Hodgkin lymphoma (B‐NHL) is the most frequent hematological malignancy. Although refined chemotherapy regimens and several new therapeutics including rituximab, a chimeric anti‐CD20 monoclonal antibody, have improved its prognosis in recent decades, there are still a substantial number of patients with chemorefractory B‐NHL. Anti‐CD19 chimeric antigen receptor (CAR) T‐cell therapy is expected to be an effective adoptive cell treatment and has the potential to overcome the chemorefractoriness of B‐cell leukemia and lymphoma. Recently, several clinical trials have shown remarkable efficacy of anti‐CD19 CAR T‐cell therapy, not only in B‐acute lymphoblastic leukemia but also in B‐NHL. Nonetheless, there are several challenges to overcome before introduction into clinical practice, such as: (i) further refinement of the manufacturing process, (ii) further improvement of efficacy, (iii) finding the optimal infusion cell dose, (iv) optimization of lymphocyte‐depleting chemotherapy, (v) identification of the best CAR structure, and (vi) optimization of toxicity management including cytokine release syndrome, neurologic toxicity, and on‐target off‐tumor toxicity. Several ways to solve these problems are currently under study. In this review, we describe the updated clinical data regarding anti‐CD19 CAR T‐cell therapy, with a focus on B‐NHL, and discuss the clinical implications and perspectives of CAR T‐cell therapy.

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Development and Use of the Anti-CD19 Chimeric Antigen Receptor T-Cell Therapy Axicabtagene Ciloleucel in Large B-Cell Lymphoma

Locke

Neelapu

2020

JAMA Oncol

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xicabtagene ciloleucel is an autologous, anti-CD19 chimeric antigen receptor (CAR) T-cell therapy with significantly improved efficacy in patients with refractory large B-cell lymphoma (LBCL) compared with other currently available treatment options. 1 Although standard-of-care therapies can cure approximately 60% of patients with newly diagnosed diffuse large B-cell lymphoma (DLBCL), 2,3 outcomes for patients with relapsed or refractory LBCL are poor. 4-8 A large, international, retrospective patient-level analysis of outcomes in refractory LBCL prior to the availability of CAR T-cell therapy, SCHOLAR-1, reported an objective response rate (ORR) of 26%, a complete response (CR) rate of 7%, and a short median overall survival of 6.3 months, 1 highlighting the need for innovative therapeutic approaches.The antigen CD19 is an optimal target for CAR T-cell therapy given its expression across a wide range of B-cell cancers and its restricted expression in healthy tissues. 9,10 However, targeting CD19 can lead to B-cell aplasia and hypogammaglobulinemia, similar to routinely used CD20-targeting monoclonal antibody therapies, and immunoglobulin supplementation can mitigate the increased risk of infections attributable to B-cell aplasia. 11 B-cell recovery has been observed 2 years after receiving anti-CD19 CAR T-cell therapy in patients with ongoing CR. 12 The cell product that became axicabtagene ciloleucel was collaboratively developed with Kite, a Gilead Company, and the National Cancer Institute (Figure 1A). [13][14][15][16][17] Early work revealed that, although first-generation CAR T cells (ie, CARs with only a single T-cell signaling domain) demonstrated cytotoxic activity, they lacked functional persistence. [18][19][20] For optimal T-cell activity, antigen recognition must occur in conjunction with appropriate costimulation, such as through CD28. 21 In 2009, Kochenderfer and colleagues 22 described the development of the CAR construct used in axicabtagene ciloleucel, which consists of an extracellular CD19-targeting, single-chain variable fragment, an intracellular CD28 costimulatory domain, and a CD3ζ signaling domain (Figure 1B). This development was quickly followed in 2010 by, to our knowledge, the first reported successful use of this CAR in a patient with B-cell lymphoma. 13 Additional studies from the National Cancer Institute using the CD19-CD28-CD3ζ CAR demonstrated the importance of conditioning IMPORTANCE Axicabtagene ciloleucel, an anti-CD19-CD28-CD3ζ chimeric antigen receptor T-cell therapy, was the first US Food and Drug Administration-approved, genetically engineered T-cell therapy for adults with relapsed or refractory large B-cell lymphoma (LBCL) after 2 or more lines of systemic therapy. There has not been a US Food and Drug Administration-approved product for these cancers in more than 4 decades.OBSERVATIONS Unlike traditional anticancer therapies, axicabtagene ciloleucel is a patient-specific, live-cell product that has unique requirements for manufacturing, shipping, and storage, as we...

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Kte-C19 (anti-CD19 CAR T Cells) Induces Complete Remissions in Patients with Refractory Diffuse Large B-Cell Lymphoma (DLBCL): Results from the Pivotal Phase 2 Zuma-1

Cited by 39 publications

References 0 publications

A review of cancer immunotherapy toxicity

A review of cancer immunotherapy toxicity

Clinical development of anti‐CD19 chimeric antigen receptor T‐cell therapy for B‐cell non‐Hodgkin lymphoma

Development and Use of the Anti-CD19 Chimeric Antigen Receptor T-Cell Therapy Axicabtagene Ciloleucel in Large B-Cell Lymphoma

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