Development of STEAP1 Targeting Chimeric Antigen Receptor for Adoptive Cell Therapy Against Cancer

Overview

Journal Mol Ther Oncolytics

Publisher Cell Press

Date 2022 Jul 21

PMID 35860008

Authors

Yixin Jin

Kristina Berg Lorvik

Yang Jin

Carole Beck

Adam Sike

Irene Persiconi

Emilie Kvaloy

Fahri Saatcioglu

Claire Dunn

Jon Amund Kyte

Affiliations

Soon will be listed here.

Abstract

Chimeric antigen receptors (CARs) that retarget T cells against CD19 show clinical efficacy against B cell malignancies. Here, we describe the development of a CAR against the six-transmembrane epithelial antigen of prostate-1 (STEAP1), which is expressed in ∼90% of prostate cancers, and subgroups of other malignancies. STEAP1 is an attractive target, as it is associated with tumor invasiveness and progression and only expressed at low levels in normal tissues, apart from the non-vital prostate gland. We identified the antibody coding sequences from a hybridoma and designed a CAR that is efficiently expressed in primary T cells. The T cells acquired the desired anti-STEAP1 specificity, with a polyfunctional response including production of multiple cytokines, proliferation, and the killing of cancer cells. The response was observed for both CD4 and CD8 T cells, and against all STEAP1 target cell lines tested. We evaluated the CAR T activity in both subcutaneous and metastatic xenograft mouse models of prostate cancer. Here, the CAR T cells infiltrated tumors and significantly inhibited tumor growth and extended survival in a STEAP1-dependent manner. We conclude that the STEAP1 CAR exhibits potent and functionality and can be further developed toward potential clinical use.

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