Multi-armored allogeneic MUC1 CAR T cells enhance efficacy and safety in triple-negative breast cancer

Author:

Erler Piril1ORCID,Kurcon Tomasz1,Cho Hana1ORCID,Skinner Jordan1ORCID,Dixon Chantel1,Grudman Steven1ORCID,Rozlan Sandra2,Dessez Emilie2,Mumford Ben1,Jo Sumin1ORCID,Boyne Alex1ORCID,Juillerat Alexandre1ORCID,Duchateau Philippe2ORCID,Poirot Laurent2,Aranda-Orgilles Beatriz1ORCID

Affiliation:

1. Cellectis Inc., New York, NY, USA.

2. Cellectis SA, Paris, France.

Abstract

Solid tumors, such as triple-negative breast cancer (TNBC), are biologically complex due to cellular heterogeneity, lack of tumor-specific antigens, and an immunosuppressive tumor microenvironment (TME). These challenges restrain chimeric antigen receptor (CAR) T cell efficacy, underlining the importance of armoring. In solid cancers, a localized tumor mass allows alternative administration routes, such as intratumoral delivery with the potential to improve efficacy and safety but may compromise metastatic-site treatment. Using a multi-layered CAR T cell engineering strategy that allowed a synergy between attributes, we show enhanced cytotoxic activity of MUC1 CAR T cells armored with PD1 KO , tumor-specific interleukin-12 release, and TGFBR2 KO attributes catered towards the TNBC TME. Intratumoral treatment effectively reduced distant tumors, suggesting retention of antigen-recognition benefits at metastatic sites. Overall, we provide preclinical evidence of armored non-alloreactive MUC1 CAR T cells greatly reducing high TNBC tumor burden in a TGFB1- and PD-L1–rich TME both at local and distant sites while preserving safety.

Publisher

American Association for the Advancement of Science (AAAS)

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