Enhancing the specificity of T-cell cultures for adoptive immunotherapy of cancer

Author:

Duong Connie PM1,Westwood Jennifer A1,Berry Linda J1,Darcy Phillip K123,Kershaw Michael H

Affiliation:

1. Cancer Immunology Research Program, Peter MacCallum Cancer Center, St Andrews Place, Melbourne, Victoria 3002, Australia

2. Department of Pathology, University of Melbourne, Victoria, Australia

3. Department of Immunology, Monash University, Clayton, Victoria, Australia

Abstract

Adoptive immunotherapy is a promising approach for the treatment of cancer; however, autoimmunity against normal tissue can be a serious complication of this therapy. We hypothesized that T-cell cultures responding maximally only when engaging two antigens would be more specific for tumor cells, and less active against normal cells, as long as the tumor expressed both antigens, while normal cells expressed only one of the antigens. A model system was developed consisting of cell lines expressing either folate binding protein or erbB-2, representing ‘normal’ tissue, and cells expressing both antigens representing tumor tissue. Human T-cell cultures were produced using two chimeric antigen receptor vectors (‘dual transduced’), or using a single chimeric antigen receptor vector (monospecific). Dual-transduced T cells responded less against ‘normal’ cells compared with tumor cells. This relatively simple procedure produced T-cell cultures that were as active against a tumor as the monospecific cultures used traditionally, but had lower activity against model normal cells.

Publisher

Future Medicine Ltd

Subject

Oncology,Immunology,Immunology and Allergy

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