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. 2021 Dec;9(12):1425-1438.
doi: 10.1158/2326-6066.CIR-20-0837. Epub 2021 Oct 22.

CAR T-cell Entry into Tumor Islets Is a Two-Step Process Dependent on IFNγ and ICAM-1

Chahrazade Kantari-Mimoun  1   2 Sarah Barrin  1   2 Lene Vimeux  1   2 Sandrine Haghiri  1   2 Claire Gervais  1   2 Sandy Joaquina  1   2 Joerg Mittelstaet  3 Nadine Mockel-Tenbrinck  3 Ali Kinkhabwala  3 Diane Damotte  4   5 Audrey Lupo  4   5 Mathilde Sibony  4 Marco Alifano  6 Elisabetta Dondi  7 Nadège Bercovici  1   2 Alain Trautmann  1   2 Andrew D Kaiser  3 Emmanuel Donnadieu  8   2
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CAR T-cell Entry into Tumor Islets Is a Two-Step Process Dependent on IFNγ and ICAM-1

Chahrazade Kantari-Mimoun et al. Cancer Immunol Res. 2021 Dec.

Abstract

Adoptive transfer of T cells expressing chimeric antigen receptors (CAR) has shown remarkable clinical efficacy against advanced B-cell malignancies but not yet against solid tumors. Here, we used fluorescent imaging microscopy and ex vivo assays to compare the early functional responses (migration, Ca2+, and cytotoxicity) of CD20 and EGFR CAR T cells upon contact with malignant B cells and carcinoma cells. Our results indicated that CD20 CAR T cells rapidly form productive ICAM-1-dependent conjugates with their targets. By comparison, EGFR CAR T cells only initially interacted with a subset of carcinoma cells located at the periphery of tumor islets. After this initial peripheral activation, EGFR CAR T cells progressively relocated to the center of tumor cell regions. The analysis of this two-step entry process showed that activated CAR T cells triggered the upregulation of ICAM-1 on tumor cells in an IFNγ-dependent pathway. The ICAM-1/LFA-1 interaction interference, through antibody or shRNA blockade, prevented CAR T-cell enrichment in tumor islets. The requirement for IFNγ and ICAM-1 to enable CAR T-cell entry into tumor islets is of significance for improving CAR T-cell therapy in solid tumors.

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