Multiplex Genome Editing As a Platform for “Off-the-Shelf” Adoptive CAR T-Cell Immunotherapies

Derniame, Sophie; Zhan, Hong; Poirot, Laurent; Schiffer-Mannioui, Cécile; Galetto, Román; Beurdeley, Marine; Reynier, Stephan; Arnould, Sylvain; Qasim, Waseem; Smith, Julianne

doi:10.1182/blood.v124.21.1111.1111

Cited by 3 publications

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“…Through lentiviral transduction, expression of a single chain variable fragment (scFv) targeting CD19 and linked to CD137 (4‐1BB) and CD3ζ co‐stimulatory/signalling domains is achieved in GMP grade. Importantly, the starting material are healthy donor peripheral blood mononuclear cells (PBMCs) [63,64]. Additionally, UCART19 offers an enhanced safety profile over earlier therapies as the anti‐CD19 scFv‐41BB‐CD3ζ is linked to an epitope marker/suicide gene (RQR8) that encodes target epitopes from CD34 and CD20, thereby allowing purification of the engineered population via CliniMACS ® CD34 selection.…”

Section: Clinical Trials With Talen Technologymentioning

confidence: 99%

The clinical potential of gene editing as a tool to engineer cell‐based therapeutics

Ashmore-Harris

Fruhwirth

2020

Clinical & Translational Med

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The clinical application of ex vivo gene edited cell therapies first began a decade ago with zinc finger nuclease editing of autologous CD4+ T‐cells. Editing aimed to disrupt expression of the human immunodeficiency virus co‐receptor gene CCR5, with the goal of yielding cells resistant to viral entry, prior to re‐infusion into the patient. Since then the field has substantially evolved with the arrival of the new editing technologies transcription activator‐like effector nucleases (TALENs) and clustered regularly interspaced short palindromic repeats (CRISPR), and the potential benefits of gene editing in the arenas of immuno‐oncology and blood disorders were quickly recognised. As the breadth of cell therapies available clinically continues to rise there is growing interest in allogeneic and off‐the‐shelf approaches and multiplex editing strategies are increasingly employed. We review here the latest clinical trials utilising these editing technologies and consider the applications on the horizon.

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Section: Clinical Trials With Talen Technologymentioning

confidence: 99%

The clinical potential of gene editing as a tool to engineer cell‐based therapeutics

Ashmore-Harris

Fruhwirth

2020

Clinical & Translational Med

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Manufacturing Cell Therapies Using Engineered Biomaterials

Abdeen

Saha

2017

Trends in Biotechnology

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Emerging manufacturing processes to generate advanced regenerative cell therapies involve extensive genomic and/or epigenomic manipulation of autologous or allogeneic cells. These cell engineering processes need to be carefully controlled and standardized in order to maximize safety and efficacy in clinical trials. Engineered biomaterials with smart and tunable properties offer an intriguing tool to provide or deliver cues to retain stemness, direct differentiation, promote reprogramming, manipulate the genome, or select functional phenotypes. This review discusses the use of engineered biomaterials to control human cell manufacturing. Future work exploiting engineered biomaterials has the potential to generate manufacturing processes that produce standardized cells with well-defined critical quality attributes appropriate for clinical testing.

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Novel immunotherapies in lymphoid malignancies

et al. 2015

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The success of the anti-CD20 monoclonal antibody rituximab in the treatment of lymphoid malignancies provided proof-of-principle for exploiting the immune system therapeutically. Since the FDA approval of rituximab in 1997, several novel strategies that harness the ability of T cells to target cancer cells have emerged. Reflecting on the promising clinical efficacy of these novel immunotherapy approaches, the FDA has recently granted ‘breakthrough’ designation to three novel treatments with distinct mechanisms. First, chimeric antigen receptor (CAR)-T-cell therapy is promising for the treatment of adult and paediatric relapsed and/or refractory acute lymphoblastic leukaemia (ALL). Second, blinatumomab, a bispecific T-cell engager (BiTE®) antibody, is now approved for the treatment of adults with Philadelphia-chromosome-negative relapsed and/or refractory B-precursor ALL. Finally, the monoclonal antibody nivolumab, which targets the PD-1 immune-checkpoint receptor with high affinity, is used for the treatment of Hodgkin lymphoma following treatment failure with autologous-stem-cell transplantation and brentuximab vedotin. Herein, we review the background and development of these three distinct immunotherapy platforms, address the scientific advances in understanding the mechanism of action of each therapy, and assess the current clinical knowledge of their efficacy and safety. We also discuss future strategies to improve these immunotherapies through enhanced engineering, biomarker selection, and mechanism-based combination regimens.

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Multiplex Genome Editing As a Platform for “Off-the-Shelf” Adoptive CAR T-Cell Immunotherapies

Cited by 3 publications

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The clinical potential of gene editing as a tool to engineer cell‐based therapeutics

The clinical potential of gene editing as a tool to engineer cell‐based therapeutics

Manufacturing Cell Therapies Using Engineered Biomaterials

Novel immunotherapies in lymphoid malignancies

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