Engineered Microglia‐Exosomes Coated Highly Twisting AIE Photothermal Agents to Efficiently Cross Blood‐Brain‐Barrier for Mild Photothermal‐Immune Checkpoint Blockade Therapy in Glioblastoma

Author:

Lin Xun1,Sun Zhihong2,Huang Shiyun1,Liu Chuyao1,Peng Jin1,Li Yueying1,Xiong Yue1,Gao Hong1,Chen Jianwei1,Qi Junyang1,Sun Chengming2,Cai Lintao34,Deng Guanjun1ORCID,Deng Wenbin15

Affiliation:

1. School of Pharmaceutical Sciences (Shenzhen) Shenzhen Campus of Sun Yat‐sen University Shenzhen 518107 P. R. China

2. The Affiliated Yantai Yuhuangding Hospital of Qingdao University Yantai 264000 P. R. China

3. Sino‐Euro Center of Biomedicine and Health Shenzhen 518024 P. R. China

4. Guangdong Key Laboratory of Nanomedicine CAS-HK Joint Lab for Biomaterials CAS Key Laboratory of Biomedical Imaging Science and System Shenzhen Institute of Advanced Technology Chinese Academy of Sciences Shenzhen 518055 P.R. China

5. Department of Biochemistry and Molecular Medicine School of Medicine University of California at Davis Sacramento CA 95817 USA

Abstract

AbstractImmune checkpoint blockade (ICB) therapy has achieved remarkable therapeutic effects in cancer, but it is not effective in glioblastoma (GBM). The main reason is that it is difficult for drugs to penetrate blood‐brain‐barrier (BBB) to GBM and lacks enough pre‐existing cytotoxic CD8+ T cells in GBM microenvironment. Here, two AIE photothermal agents (Fs and Fo) are synthesized with NIR‐II fluorescence emission and increase molecular twisting of AIE photothermal agents by simply changing one O atom into S atom, improving Fs photothermal conversion efficiency to 48%. Subsequently, engineered microglia‐exosomes AIE nanoparticles (EE@Fs‐NPs) are prepared by encapsulating Fs with microglia‐exosomes which express immune checkpoint LAG3 inhibitory antibody (anti‐LAG3) via genetic engineering technology. Engineered microglia‐exosomes endow that EE@Fs‐NPs cross BBB and target GBM, which successfully deliver anti‐LAG3 to GBM. Anti‐LAG3 highly reverses T cells exhaustion and generates TNF‐α for inhibiting the expression of heat shock proteins to enhance tumor cells thermosensitivity. Moreover, AIE photothermal agents of EE@Fs‐NPs generate mild photothermal therapy to destroy tumor cells and improve the infiltration of cytotoxic CD8+ T cells in GBM, which increases the responsiveness of ICB therapy. EE@Fs‐NPs produce powerful mild photothermal‐immune synergistic therapeutic effect, which will provide a therapeutic platform for the efficient treatment of GBM.

Funder

National Natural Science Foundation of China

Shenzhen Science and Technology Innovation Program

Basic and Applied Basic Research Foundation of Guangdong Province

Natural Science Foundation of Shandong Province

Publisher

Wiley

Subject

Electrochemistry,Condensed Matter Physics,Biomaterials,Electronic, Optical and Magnetic Materials

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