S1635 Academic, Phase1 Trial on T Cells Expressing Both Cd19 Chimeric Antigen Receptor and Inducible Caspase 9 Safety Switch for Treatment of Childhood Acute Lymphoblastic Leukaemia and Non‐hodgkin Lymphoma

Bufalo, Francesca Del; Merli, Pietro; Vinti, Luciana; Algeri, Mattia; Cefalo, Maria Giuseppina; Bertaina, Valentina; Pira, Giuseppina Li; Caruana, Ignazio; Angelis, Biagio De; Boffa, Iolanda; Cecca, S. De; Orlando, Domenico; Guercio, Marika; Sinibaldi, Matilde; Abbaszadeh, Zeinab; Polito, Vinicia Assunta; Cristantielli, Rosaria; Quintarelli, Concetta; Locatelli, F.

doi:10.1097/01.hs9.0000564788.37982.52

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“…iCasp9-CD19.CAR-T cells were also evaluated in an academic, phase I/II trial enrolling pediatric patients with B-ALL or B-cell NHL. CRS occurred in 58.8% of patients, but reached grade 3 only in one subject, and no life-threatening adverse events requiring iCasp9 safety switch activation were noted (93).…”

Section: Clinical Trials Evaluating Off-switch Platformsmentioning

confidence: 92%

Fully equipped CARs to address tumor heterogeneity, enhance safety, and improve the functionality of cellular immunotherapies

Alviano,

Biondi,

Grassenis

et al. 2024

Front. Immunol.

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Although adoptive transfer of chimeric antigen receptor (CAR)-engineered T cells has achieved unprecedented response rates in patients with certain hematological malignancies, this therapeutic modality is still far from fulfilling its remarkable potential, especially in the context of solid cancers. Antigen escape variants, off-tumor destruction of healthy tissues expressing tumor-associated antigens (TAAs), poor CAR-T cell persistence, and the occurrence of functional exhaustion represent some of the most prominent hurdles that limit CAR-T cell ability to induce long-lasting remissions with a tolerable adverse effect profile. In this review, we summarize the main approaches that have been developed to face such bottlenecks, including the adapter CAR (AdCAR) system, Boolean-logic gating, epitope editing, the modulation of cell-intrinsic signaling pathways, and the incorporation of safety switches to precisely control CAR-T cell activation. We also discuss the most pressing issues pertaining to the selection of co-stimulatory domains, with a focus on strategies aimed at promoting CAR-T cell persistence and optimal antitumor functionality.

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Section: Clinical Trials Evaluating Off-switch Platformsmentioning

confidence: 92%