Spatiotemporal Controllable Sono‐Nanovaccines Driven by Free‐Field Based Whole‐Body Ultrasound for Personalized Cancer Therapy

Author:

Wang Yang1,Li Guangzhe2ORCID,Su Jianlong1,Liu Yiming1,Zhang Xiaomai1,Zhang Guanyi1,Wu Zhihao1,Li Jinrong1,Zhang Yuxuan1,Wang Xu1,Yang Zejia1,Wang Ruimin1,Wang Chengdong3,Wang Liu2,Sun Fangfang3,Zhao Weijie2,Wang Xuejian4,Peng Xiaojun1,Shao Kun1ORCID

Affiliation:

1. State Key Laboratory of Fine Chemicals School of Chemical Engineering Dalian University of Technology Dalian 116024 China

2. State Key Laboratory of Fine Chemicals Department of Pharmacy School of Chemical Engineering Dalian University of Technology Dalian 116024 China

3. Nuclear Medicine First Affiliated Hospital of Dalian Medical University Dalian 116021 China

4. Department of Urology First Affiliated Hospital of Dalian Medical University Dalian 116021 China

Abstract

AbstractTherapeutic cancer vaccines fail to produce satisfactory outcomes against solid tumors since vaccine‐induced anti‐tumor immunity is significantly hampered by immunosuppression. Generating an in situ cancer vaccine targeting immunological cold tumor microenvironment (TME) appears attractive. Here, a type of free‐field based whole‐body ultrasound (US)‐driven nanovaccines are constructed, named G5‐CHC‐R, by conjugating the sonosensitizer, Chenghai chlorin (CHC) and the immunomodulator, resiquimod (R848) on top of a super small‐sized dendrimeric nanoscaffold. Once entering tumors, R848 can be cleaved from a hypoxia‐sensitive linker, thus modifying the TME via converting macrophage phenotypes. The animals bearing orthotopic pancreatic cancer with intestinal metastasis and breast cancer with lung metastasis are treated with G5‐CHC‐R under a free‐field based whole‐body US system. Benefit from the deep penetration capacity and highly spatiotemporal selectiveness, G5‐CHC‐R triggered by US represented a superior alternative for noninvasive irradiation of deep‐seated tumors and magnification of local immune responses via driving mass release of tumor antigens and “cold‐warm‐hot” three‐state transformation of TME. In addition to irradiating primary tumors, a robust adaptive anti‐tumor immunity is potentiated, leading to successful induction of systemic tumor suppression. The sono‐nanovaccines with good biocompatibility posed wide applicability to a broad spectrum of tumors, revealing immeasurable potential for translational research in oncology.

Funder

National Natural Science Foundation of China

Fundamental Research Funds for the Central Universities

Publisher

Wiley

Subject

General Physics and Astronomy,General Engineering,Biochemistry, Genetics and Molecular Biology (miscellaneous),General Materials Science,General Chemical Engineering,Medicine (miscellaneous)

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