Synthetic cytokine circuits that drive T cells into immune-excluded tumors

Greg M. Allen; Nicholas Frankel; Nishith R. Reddy; Hersh K. Bhargava; Maia A. Yoshida; Sierra R. Stark; Megan Purl; Jungmin Lee; Jacqueline L. Yee; Wei Yu; Aileen W. Li; K. Christopher García; Hana El‐Samad; Kole T. Roybal; Matthew H. Spitzer; Wendell A. Lim

doi:10.1126/science.aba1624

Synthetic cytokine circuits that drive T cells into immune-excluded tumors

Greg M. Allen(University of California, San Francisco), Nicholas Frankel(University of California, San Francisco), Nishith R. Reddy(University of California, San Francisco), Hersh K. Bhargava(University of California, San Francisco), Maia A. Yoshida(University of California, San Francisco), Sierra R. Stark(University of California, San Francisco), Megan Purl(University of California, San Francisco), Jungmin Lee(University of California, San Francisco), Jacqueline L. Yee(University of California, San Francisco), Wei Yu(University of California, San Francisco), Aileen W. Li(University of California, San Francisco), K. Christopher García(Howard Hughes Medical Institute), Hana El‐Samad(University of California, San Francisco), Kole T. Roybal(University of California, San Francisco), Matthew H. Spitzer(University of California, San Francisco), Wendell A. Lim(University of California, San Francisco)

Science

December 15, 2022

10.1126/science.aba1624

Cited by 219Open Access

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Abstract

Chimeric antigen receptor (CAR) T cells are ineffective against solid tumors with immunosuppressive microenvironments. To overcome suppression, we engineered circuits in which tumor-specific synNotch receptors locally induce production of the cytokine IL-2. These circuits potently enhance CAR T cell infiltration and clearance of immune-excluded tumors, without systemic toxicity. The most effective IL-2 induction circuit acts in an autocrine and T cell receptor (TCR)- or CAR-independent manner, bypassing suppression mechanisms including consumption of IL-2 or inhibition of TCR signaling. These engineered cells establish a foothold in the target tumors, with synthetic Notch-induced IL-2 production enabling initiation of CAR-mediated T cell expansion and cell killing. Thus, it is possible to reconstitute synthetic T cell circuits that activate the outputs ultimately required for an antitumor response, but in a manner that evades key points of tumor suppression.

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