Camelid‐derived Tcell engagers harnessing human γδ T cells as promising antitumor immunotherapeutic agents

Author:

Boutin Lola123ORCID,Barjon Clément4,Chauvet Morgane124,Lafrance Laura12,Senechal Eric3,Bourges Dorothée4,Vigne Emmanuelle3ORCID,Scotet Emmanuel12ORCID

Affiliation:

1. Nantes Université, Inserm UMR 1307, CNRS UMR 6075 Université d'Angers CRCI2NA Nantes France

2. LabEx IGO “Immunotherapy, Graft, Oncology” Nantes France

3. Sanofi, Large Molecule Research Vitry‐sur‐Seine France

4. Sanofi, Oncology Vitry‐sur‐Seine France

Abstract

AbstractIn the last decade, there has been a surge in developing immunotherapies to enhance the immune system's ability to eliminate tumor cells. Bispecific antibodies known as T cell engagers (TCEs) present an attractive strategy in this pursuit. TCEs aim to guide cytotoxic T cells toward tumor cells, thereby inducing a strong activation and subsequent tumor cell lysis. In this study, we investigated the activity of different TCEs on both conventional alpha‐beta (αβ) T cells and unconventional gamma delta (γδ) T cells. TCEs were built using camelid single‐domain antibodies (VHHs) targeting the tumor‐associated antigen CEACAM5 (CEA), together with T cell receptor chains or a CD3 domain. We show that Vγ9Vδ2 T cells display stronger in vitro antitumor activity than αβ T cells when stimulated with a CD3xCEA TCE. Furthermore, restricting the activation of fresh human peripheral T cells to Vγ9Vδ2 T cells limited the production of protumor factors and proinflammatory cytokines, commonly associated with toxicity in patients. Taken together, our findings provide further insights that γδ T cell‐specific TCEs hold promise as specific, effective, and potentially safe molecules to improve antitumor immunotherapies.

Funder

Fondation pour la Recherche Médicale

Sanofi

Association Nationale de la Recherche et de la Technologie

Publisher

Wiley

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