An oncolytic adenovirus coding for a variant interleukin 2 cytokine improves response to chemotherapy through enhancement of effector lymphocyte cytotoxicity, fibroblast compartment modulation and mitotic slippage

Santeri Pakola; Dafne C A Quixabeira; Tatiana V Kudling; James H A Clubb; Susanna Grönberg-Vähä-Koskela; Saru Basnet; Elise Jirovec; Victor Arias; Lyna Haybout; Camilla Heiniö; Joao M Santos; Victor Cervera-Carrascon; Riikka Havunen; Marjukka Anttila; Akseli Hemminki

doi:10.3389/fimmu.2023.1171083

An oncolytic adenovirus coding for a variant interleukin 2 cytokine improves response to chemotherapy through enhancement of effector lymphocyte cytotoxicity, fibroblast compartment modulation and mitotic slippage

Front Immunol. 2023 Jul 5:14:1171083. doi: 10.3389/fimmu.2023.1171083. eCollection 2023.

Authors

Santeri Pakola¹, Dafne C A Quixabeira^{1

2}, Tatiana V Kudling¹, James H A Clubb^{1

2}, Susanna Grönberg-Vähä-Koskela^{1

3}, Saru Basnet¹, Elise Jirovec^{1

2}, Victor Arias¹, Lyna Haybout^{1

2}, Camilla Heiniö¹, Joao M Santos^{1

2}, Victor Cervera-Carrascon^{1

2}, Riikka Havunen^{1

2}, Marjukka Anttila⁴, Akseli Hemminki^{1

2

3}

Affiliations

¹ Cancer Gene Therapy Group, Translational Immunology Research Program, University of Helsinki, Helsinki, Finland.
² TILT Biotherapeutics Ltd., Helsinki, Finland.
³ Helsinki University Hospital Comprehensive Cancer Center, Helsinki, Finland.
⁴ Pathology, Finnish Food Authority, Helsinki, Finland.

Abstract

Pancreatic ductal adenocarcinoma (PDAC) is a highly treatment-resistant cancer. Currently, the only curative treatment for PDAC is surgery, but most patients are diagnosed with metastatic disease and thus outside the scope of surgery. The majority of metastatic patients receive chemotherapy, but responses are limited. New therapeutics are thus urgently needed for PDAC. One major limitation in treating PDAC has been the highly immunosuppressive tumor microenvironment (TME) which inhibits anti-cancer immune responses. We have constructed an oncolytic adenovirus coding for a variant the interleukin 2 molecule, Ad5/3-E2F-d24-vIL2 (also known as TILT-452, and "vIL-2 virus"), with preferential binding to IL-2 receptors on the surface of effector lymphocytes over T regulatory cells (T regs). In the present study this virus was evaluated in combination with nab-paclitaxel and gemcitabine chemotherapy in Panc02 mouse model. Ad5/3-E2F-d24-vIL2 showed marked PDAC cell killing in vitro, alongside induction of mitotic slippage and immunogenic cell death in PDAC cell lines, when combined with chemotherapy. Increased survival was seen in vivo with 80% of animals surviving long term, when compared to chemotherapy alone. Moreover, combination therapy mediated enhanced tumor growth control, without observable toxicities in internal organs or external features. Survival and tumor control benefits were associated with activation of tumor infiltrating immune cells, downregulation of inhibitory signals, change in fibroblast populations in the tumors and changes in intratumoral cytokines, with increased chemokine amounts (CCL2, CCL3, CCL4) and anti-tumor cytokines (IFN-γ and TNFα). Furthermore, vIL-2 virus in combination with chemotherapy efficiently induced tumor protection upon rechallenge, that was extended to a previously non-encountered cancer cell line. In conclusion, Ad5/3-E2F-d24-vIL2 is a promising immunotherapy candidate when combined with nab-paclitaxel and gemcitabine.

Keywords: adenovirus; chemotherapy; immunotherapy; interleukin 2; oncolytic virus.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adenoviridae
Adenoviridae Infections*
Animals
Carcinoma, Pancreatic Ductal* / drug therapy
Carcinoma, Pancreatic Ductal* / therapy
Cell Line, Tumor
Cytokines / therapeutic use
Fibroblasts / pathology
Gemcitabine
Interleukin-2 / genetics
Interleukin-2 / pharmacology
Interleukin-2 / therapeutic use
Lymphocytes / pathology
Mice
Pancreatic Neoplasms*
Tumor Microenvironment

Substances

Cytokines
Interleukin-2
Gemcitabine

Grants and funding

This work was supported by MD-PhD Program of the Faculty of Medicine (University of Helsinki), Suomen Kulttuurirahasto, Jane and Aatos Erkko Foundation, HUCH Research Funds (VTR), Finnish Cancer Organizations, Sigrid Juselius Foundation, University of Helsinki, Novo Nordisk Foundation, Päivikki and Sakari Sohlberg Foundation, Finnish Red Cross Blood Service, European Union’s Horizon 2020 STACCATO Research and Innovation Programme under the Marie Skłodowska-Curie grant agreement (No 813453). We thank Albert Ehrnrooth and Karl Fazer for research support. This study received funding from TILT Biotherapeutics Ltd. The funder was not involved in the study design, collection, analysis, interpretation of data, the writing of this article or the decision to submit it for publication.