Enhanced CAR–T cell activity against solid tumors by vaccine boosting through the chimeric receptor

Leyuan Ma(Howard Hughes Medical Institute), Tanmay Dichwalkar(Massachusetts Institute of Technology), Jason Y.H. Chang(Massachusetts Institute of Technology), Benjamin Cossette(Massachusetts Institute of Technology), Daniel Garafola(Massachusetts Institute of Technology), Angela Q. Zhang(Massachusetts Institute of Technology), Michael Fichter(Massachusetts Institute of Technology), Chensu Wang(Massachusetts Institute of Technology), Simon Liang(Massachusetts Institute of Technology), Murillo Silva(Massachusetts Institute of Technology), Sudha Kumari(Massachusetts Institute of Technology), Naveen K. Mehta(Massachusetts Institute of Technology), Wuhbet Abraham(Massachusetts Institute of Technology), Nikki Thai(Massachusetts Institute of Technology), Na Li(Massachusetts Institute of Technology), K. Dane Wittrup(Massachusetts Institute of Technology), Darrell J. Irvine(Howard Hughes Medical Institute)
Science
July 12, 2019
Cited by 425Open Access
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Abstract

Chimeric antigen receptor-T cell (CAR-T) therapy has been effective in the treatment of hematologic malignancies, but it has shown limited efficacy against solid tumors. Here we demonstrate an approach to enhancing CAR-T function in solid tumors by directly vaccine-boosting donor cells through their chimeric receptor in vivo. We designed amphiphile CAR-T ligands (amph-ligands) that, upon injection, trafficked to lymph nodes and decorated the surfaces of antigen-presenting cells, thereby priming CAR-Ts in the native lymph node microenvironment. Amph-ligand boosting triggered massive CAR-T expansion, increased donor cell polyfunctionality, and enhanced antitumor efficacy in multiple immunocompetent mouse tumor models. We demonstrate two approaches to generalizing this strategy to any chimeric antigen receptor, enabling this simple non-human leukocyte antigen-restricted approach to enhanced CAR-T functionality to be applied to existing CAR-T designs.


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