Gemcitabine‐Loaded Injectable Hydrogel for Localized Breast Cancer Immunotherapy

Author:

Barough Mahdieh Shokrollahi123,Seyfoori Amir34,Askari Esfandyar34,Mahdavi Mehdi1,Sarrami Forooshani Ramin1,Sadeghi Behnam5,Kazemi Mohammad Hossein26,Falak Reza27,Khademhosseini Ali8,Mojtabavi Nazanin2,Akbari Mohsen348ORCID

Affiliation:

1. ATMP Department Breast Cancer Research Center Motamed Cancer Institute ACECR Tehran 1517964311 Iran

2. Department of Immunology School of Medicine Iran University of Medical Sciences Tehran 1449614535 Iran

3. Laboratory for Innovations in Micro Engineering (LiME) Department of Mechanical Engineering University of Victoria Victoria British Columbia V8P 5C2 Canada

4. Center for Advanced Materials and Related Technologies University of Victoria Victoria British Columbia V8P 5C2 Canada

5. Translational Cell Therapy Research (TCR) Division of Pediatrics Department of Clinical Science Intervention and Technology (CLINTEC) Karolinska Institutet Stockholm 14157 Sweden

6. Department of Molecular Microbiology and Immunology Keck School of Medicine University of Southern California Los Angeles CA 90033 USA

7. Immunology research center Iran University of Medical Sciences Tehran 1449614535 Iran

8. Terasaki Institute for Biomedical Innovation Los Angeles CA 90064 USA

Abstract

AbstractInjectable hydrogels for cancer immunotherapy are effective for both active and passive approaches. Tumor‐infiltrating lymphocyte (TIL) immunoshaping can change the tumor microenvironment to favor tumor cell elimination. The primary objective of immunoshaping is to reduce regulatory T‐cells (Tregs), which can enhance the effectiveness of ex vivo immune cell therapy in solid tumors. A shear‐thinning injectable hydrogel that consists of gelatin and Laponite (Gel‐Lap) is used in this study. By optimizing the formulation, their immunotherapeutic and anti‐tumor properties are examined. Gemcitabine (GEM), an anti‐metabolite cancer chemotherapy agent, is loaded into a Gel‐Lap hydrogel (immunogel). The study compares the effects of immunogel on 4T1 inoculated breast cancer animal models. Results show that immunogel increases survival rates and significantly inhibits metastasis. The Treg cell population reduction is observed up to 70% in TILs and splenocyte population in line with CD8+ T‐cells population increment in inguinal lymph nodes near the tumor region; the CD8+ T‐cells function may be mediated through overexpression of eomesodermin (EOMES) as cytotoxic T lymphocyte (CTL) activation transcription factor. The human 3D cell culture model confirmed results in animal data demonstrating T‐cell migration through the hydrogel and anticancer efficacy. Local delivery of GEM using our silicate‐based hydrogel holds promise for editing tumor microenvironment in favor of systemic immune responses.

Funder

Natural Sciences and Engineering Research Council of Canada

Canada Foundation for Innovation

Iran University of Medical Sciences

University of Victoria

Publisher

Wiley

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