NIR‐II‐Responsive Hybrid System Achieves Cascade‐Augmented Antitumor Immunity via Genetic Engineering of Both Bacteria and Tumor Cells

Author:

Dai Xiaoguang1,Liu Zhiwen1,Zhao Xiaoyi1,Guo Kangli1,Ding Xiaokang1,Xu Fu‐Jian1,Zhao Nana1ORCID

Affiliation:

1. State Key Laboratory of Chemical Resource Engineering Key Laboratory of Biomedical Materials of Natural Macromolecules Beijing Laboratory of Biomedical Materials College of Materials Sciences and Engineering Beijing University of Chemical Technology Beijing 100029 China

Abstract

AbstractThe combination of nanoparticles and tumor‐targeting bacteria for cancer immunotherapy can overcome the shortcomings of poor nanoparticle accumulation, limited penetration, and restricted distribution. However, it remains a great challenge for the hybrid system to improve therapeutic efficacy through the simultaneous and controllable regulation of immune cells and tumor cells. Herein, a hybrid therapeutic platform is rationally designed to achieve immune cascade‐augmented cancer immunotherapy. To construct the hybrids, photothermal nanoparticles responsive to light in the second near‐infrared (NIR‐II) region are conjugated onto the surface of engineered bacteria through pH‐responsive Schiff base bonds. Taking advantage of the hypoxia targeting and deep penetration characteristics of the bacteria, the hybrids can accumulate at tumor sites. Then nanoparticles detach from the bacteria to realize genetic engineering of tumor cells, which induces tumor cell apoptosis and down‐regulate the expression of programmed cell death ligand 1 to alleviate immunosuppressive tumor microenvironment. The mild photothermal heating can not only induce tumor‐associated antigen release, but also trigger sustainable expression of cytokine interleukin‐2. Notably, a synergistic antitumor effect is achieved between the process of p53 transfection and NIR‐II light‐activated genetic engineering of bacteria. This work proposes a facile strategy for the construction of hybrid system to achieve cascade‐augmented cancer immunotherapy.

Funder

National Key Research and Development Program of China

National Natural Science Foundation of China

Publisher

Wiley

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