Activatable Semiconducting Polymer Pro‐nanomodulators for Deep‐Tissue Sono‐immunotherapy of Orthotopic Pancreatic Cancer

Author:

Li Jingchao1,Yu Ningyue1,Cui Dong2,Huang Jiaguo2,Luo Yu3,Pu Kanyi2ORCID

Affiliation:

1. State Key Laboratory for Modification of Chemical Fibers and Polymer Materials College of Biological Science and Medical Engineering Donghua University Shanghai 201620 China

2. School of Chemistry Chemical Engineering and Biotechnology Lee Kong Chian School of Medicine Nanyang Technological University 70 Nanyang Drive Singapore 637457 Singapore

3. School of Chemistry and Chemical Engineering Shanghai Engineering Technology Research Center for Pharmaceutical Intelligent Equipment Shanghai University of Engineering Science Shanghai 201620 China

Abstract

AbstractImmunotherapy has provided a promising modality for cancer treatment, while it often has the issues of limited response rates and potential off‐target side effects in clinical practice. We herein report the construction of semiconducting polymer pro‐nanomodulators (SPpMs) with ultrasound (US)‐mediated activatable pharmacological actions for deep‐tissue sono‐immunotherapy of orthotopic pancreatic cancer. Such SPpMs consist of a sonodynamic semiconducting polymer backbone grafted with poly(ethylene glycol) chains linked with two immunomodulators (a programmed death‐ligand 1 blocker and an indoleamine 2,3‐dioxygenase inhibitor) via a singlet oxygen (1O2)‐cleavable segment. In view of the excellent sonodynamic property of the semiconducting polymer core, SPpMs enable effective generation of 1O2 under US treatment, even in a deep‐tissue depth up to 12 cm. The generated 1O2 not only ablates tumors via a sonodynamic effect and induces immunogenic cell death, but also destroys the 1O2‐cleavable segments to allow in situ release of immunomodulators in tumors. This synergetic action results in boosted antitumor immune response via reversing two tumor immunosuppressive pathways. As such, SPpMs mediate deep‐tissue sono‐immunotherapy to completely eradicate orthotopic pancreatic cancer and effectively prevent tumor metastasis. Moreover, such an immune activation reduces the possibility of immune‐related adverse events. This study thus provides a smart activatable nanoplatform for precise immunotherapy of deep‐seated tumors.

Publisher

Wiley

Subject

General Chemistry,Catalysis

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