Tripokin: A multi‐specific immunocytokine for cancer immunotherapy

Author:

Prodi Eleonora12,Corbellari Riccardo12,Ghezzi Lorenzo3,Ciambellotti Silvia3,Catastini Jacopo Elia3,Rappuoli Marco3,Rotta Giulia1,Sakic Irma4,Weiss Tobias4,Weller Michael4,Pellegrino Christian5,Manz Markus G.5,Neri Dario36,De Luca Roberto1ORCID

Affiliation:

1. Philochem AG Otelfingen Switzerland

2. CiBIO (Department of Cellular, Computational and Integrative Biology) University of Trento Trento Italy

3. Philogen Spa Siena Italy

4. Department of Neurology and Clinical Neuroscience Center University Hospital Zurich and University of Zurich Zurich Switzerland

5. Department of Medical Oncology and Hematology University Hospital Zurich and University of Zurich Zurich Switzerland

6. Department of Chemistry and Applied Biosciences Swiss Federal Institute of Technology (ETH Zürich) Zurich Switzerland

Abstract

AbstractAntibodies that target the tumor microenvironment can be used to deliver pro‐inflammatory payloads, such as cytokines. Cytokines are small proteins able to modulate the activity of the immune system, and antibody–cytokine fusion proteins have been tested in preclinical and clinical settings. In this study, we describe Tripokin, a novel multi‐specific fusion protein that combines interleukin‐2 and a single amino acid mutant of tumor necrosis factor. The two pro‐inflammatory payloads were fused to the L19 antibody, a clinical‐grade antibody against the extradomain B of fibronectin. The human payloads were used for clinical applications, while the corresponding murine cytokines were used for preclinical studies. The resulting fusion proteins were produced in mammalian cells and purified to homogeneity. The murine Tripokin product was well tolerated in tumor‐bearing mice at three doses of 30 μg in a 2‐day interval and promoted rapid tumor eradication in murine models, more efficiently than single‐agent immunocytokines. Tripokin induced rapid tumor necrosis and stimulated a robust immune response, impacting innate and adaptive immune pathways. In addition, the combination with immune checkpoint inhibitors further boosted the therapeutic efficacy of our molecule. Tripokin represents a promising clinical candidate for the simultaneous delivery of interleukin‐2 and tumor necrosis factor to neoplastic sites.

Funder

Innosuisse - Schweizerische Agentur für Innovationsförderung

Publisher

Wiley

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