Polymer Backpack‐Loaded Tissue Infiltrating Monocytes for Treating Cancer

Author:

Kapate Neha123,Dunne Michael12,Gottlieb Alexander P.14,Mukherji Malini12,Suja Vineeth Chandran12,Prakash Supriya12,Park Kyung Soo12,Kumbhojkar Ninad12,Guerriero Jennifer L.4567,Mitragotri Samir12ORCID

Affiliation:

1. Harvard John A. Paulson School of Engineering and Applied Sciences Harvard University Allston MA 02134 USA

2. Wyss Institute for Biologically Inspired Engineering Boston MA 02115 USA

3. Harvard‐MIT Program in Health Science and Technology Massachusetts Institute of Technology Cambridge MA 02139 USA

4. Division of Breast Surgery Department of Surgery Brigham and Women's Hospital Boston MA 02115 USA

5. Department of Medical Oncology Dana‐Farber Cancer Institute 450 Brookline Avenue Boston MA 02215 USA

6. Breast Oncology Program Dana‐Farber/Brigham and Women's Cancer Center Boston MA 02115 USA

7. Ludwig Center for Cancer Research at Harvard Harvard Medical School Boston MA 02215 USA

Abstract

AbstractAdoptive cell therapies are dramatically altering the treatment landscape of cancer. However, treatment of solid tumors remains a major unmet need, in part due to limited adoptive cell infiltration into the tumor and in part due to the immunosuppressive tumor microenvironment. The heterogeneity of tumors and presence of nonresponders also call for development of antigen‐independent therapeutic approaches. Myeloid cells offer such an opportunity, given their large presence in the immunosuppressive tumor microenvironment, such as in triple negative breast cancer. However, their therapeutic utility is hindered by their phenotypic plasticity. Here, the impressive trafficking ability of adoptively transferred monocytes is leveraged into the immunosuppressive 4T1 tumor to develop an antitumor therapy. To control monocyte differentiation in the tumor microenvironment, surface‐adherent “backpacks” stably modified with interferon gamma (IFNγ) are developed to stimulate macrophage plasticity into a pro‐inflammatory, antitumor phenotype, a strategy as referred to as Ornate Polymer backpacks on Tissue Infiltrating Monocytes (OPTIMs). Treatment with OPTIMs substantially reduces tumor burden in a mouse 4T1 model and significantly increases survival. Cytokine and immune cell profiling reveal that OPTIMs remodeled the tumor microenvironment into a pro‐inflammatory state.

Funder

National Science Foundation

Harvard School of Engineering and Applied Sciences

Publisher

Wiley

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