Constitutive Turbodomains enhance expansion and antitumor activity of allogeneic BCMA CAR T cells in preclinical models

Author:

Lin Regina J.1ORCID,Sutton Janette1ORCID,Bentley Trevor1ORCID,Vargas-Inchaustegui Diego A.1,Nguyen Duy1,Cheng Hsin-Yuan1,Yoon Hayung1,Van Blarcom Thomas J.1ORCID,Sasu Barbra J.1ORCID,Panowski Siler H.1ORCID,Sommer Cesar1ORCID

Affiliation:

1. Allogene Therapeutics Inc., 210 E. Grand Avenue, South San Francisco, CA 94080, USA.

Abstract

The magnitude of CAR T cell expansion has been associated with clinical efficacy. Although cytokines can augment CAR T cell proliferation, systemically administered cytokines can result in toxicities. To gain the benefits of cytokine signaling while mitigating toxicities, we designed constitutively active synthetic cytokine receptor chimeras (constitutive Turbodomains) that signal in a CAR T cell–specific manner. The modular design of Turbodomains enables diverse cytokine signaling outputs from a single homodimeric receptor chimera and allows multiplexing of different cytokine signals. Turbodomains containing an IL-2/15Rβ–derived signaling domain closely mimicked IL-15 signaling and enhanced CAR T cell potency. Allogeneic TurboCAR T cells targeting BCMA showed no evidence of aberrant proliferation yet displayed enhanced expansion and antitumor activity, prolonging survival and preventing extramedullary relapses in mouse models. These results illustrate the potential of constitutive Turbodomains to achieve selective potentiation of CAR T cells and demonstrate the safety and efficacy of allogeneic BCMA TurboCAR T cells, supporting clinical evaluation in multiple myeloma.

Publisher

American Association for the Advancement of Science (AAAS)

Subject

Multidisciplinary

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