Percutaneous Delivery of Oncogel for Targeted Liver Tumor Ablation and Controlled Release of Therapeutics

Author:

Albadawi Hassan1,Zhang Zefu1,Keum Hyeongseop1,Cevik Enes1,Nagalo Bolni M2,Gunduz Seyda13,Kita Hirohito4,Oklu Rahmi1ORCID

Affiliation:

1. Division of Vascular & Interventional Radiology Laboratory for Patient Inspired Engineering Mayo Clinic 13400 East Shea Blvd. Scottsdale AR 85259 USA

2. University of Arkansas for Medical Sciences College of Medicine Department of Pathology 301 West Markham Street Little Rock AR 72205 USA

3. Department of Medical Oncology Istinye University; Bahcesehir Liv Hospital Istanbul 34517 Turkey

4. Department of Immunology Division of Allergy, Asthma, and Clinical Immunology and the Department of Medicine Mayo Clinic Arizona Scottsdale AR 85259 USA

Abstract

AbstractAdvanced‐stage liver cancers are associated with poor prognosis and have limited treatment options, often leading the patient to hospice care. Percutaneous intratumoral injection of anticancer agents has emerged as a potential alternative to systemic therapy to overcome tumor barriers, increase bioavailability, potentiate immunotherapy, and avoid systemic toxicity, which advanced‐stage cancer patients cannot tolerate. Here, an injectable OncoGel (OG) comprising of a nanocomposite hydrogel loaded with an ionic liquid (IL) is developed for achieving a predictable and uniform tumor ablation and long‐term slow release of anticancer agents into the ablation zone. Rigorous mechanical, physiochemical, drug release, cytotoxicity experiments, and ex vivo human tissue testing identify an injectable version of the OG with bactericidal properties against highly resistant bacteria. Intratumoral injection of OG loaded with Nivolumab (Nivo) and doxorubicin (Dox) into highly malignant tumor models in mice, rats, and rabbits demonstrates enhanced survival and tumor regression associated with robust tissue ablation and drug distribution throughout the tumor. Mass cytometry and proteomic studies in a mouse model of colorectal cancer that often metastasizes to the liver indicate an enhanced anticancer immune response following the intratumoral injection of OG. OG may augment immunotherapy and potentially improve outcomes in liver cancer patients.

Funder

National Institutes of Health

Publisher

Wiley

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