Interferon‐expressing oncolytic adenovirus + chemoradiation inhibited pancreatic cancer growth in a hamster model

Author:

Shinoda Shuhei12ORCID,Sharma Nikita S.1,Nakamura Naohiko1,Inoko Kazuho1,Sato‐Dahlman Mizuho13,Murugan Paari4,Davydova Julia13,Yamamoto Masato135

Affiliation:

1. Department of Surgery University of Minnesota Minneapolis MN USA

2. Department of Gastroenterology and Hepatology Yamaguchi University Graduate school of Medicine Yamaguchi Japan

3. Masonic Cancer Center University of Minnesota Minneapolis MN USA

4. Department of Laboratory Medicine and Pathology University of Minnesota Minneapolis MN USA

5. Institute of Molecular Virology University of Minnesota Minneapolis MN USA

Abstract

AbstractPast clinical trials of adjuvant therapy combined with interferon (IFN) alpha, fluorouracil, cisplatin, and radiation improved the 5‐year survival rate of pancreatic ductal adenocarcinoma (PDAC). However, these trials also revealed the disadvantages of the systemic toxicity of IFN and insufficient delivery of IFN. To improve efficacy and tolerability, we have developed an oncolytic adenovirus‐expressing IFN (IFN‐OAd). Here, we evaluated IFN‐OAd in combination with chemotherapy (gemcitabine + nab‐paclitaxel) + radiation. Combination index (CI) analysis showed that IFN‐OAd + chemotherapy + radiation was synergistic (CI <1). Notably, IFN‐OAd + chemotherapy + radiation remarkably suppressed tumor growth and induced a higher number of tumor‐infiltrating lymphocytes without severe side toxic effects in an immunocompetent and adenovirus replication‐permissive hamster PDAC model. This is the first study to report that gemcitabine + nab‐paclitaxel, the current first‐line chemotherapy for PDAC, did not hamper virus replication in a replication‐permissive immunocompetent model. IFN‐OAd has the potential to overcome the barriers to clinical application of IFN‐based therapy through its tumor‐specific expression of IFN, induction of antitumor immunity, and sensitization with chemoradiation. Combining IFN‐OAd with gemcitabine + nab‐paclitaxel + radiation might be an effective and clinically beneficial treatment for PDAC patients.

Funder

National Cancer Institute

Publisher

Wiley

Subject

Cancer Research,Oncology,General Medicine

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