Self‐Cascade Nanozyme Reactor as a Cuproptosis Inducer Synergistic Inhibition of Cellular Respiration Boosting Radioimmunotherapy

Author:

Li Rui12,Zhao Weiheng1,Han Zhuo3,Feng Na4,Wu Tingting56,Xiong Huihua1,Jiang Wei56ORCID

Affiliation:

1. Department of Oncology Tongji Hospital Huazhong University of Science and Technology Wuhan 430000 China

2. Department of Respiratory Intervention The Affiliated Cancer Hospital of Zhengzhou University & Henan Cancer Hospital No.127, Dongming Road, Jinshui Zhengzhou 450008 China

3. Department of General Surgery Tangdu Hospital the Air Force Medical University Xi'an 710000 China

4. Department of Laboratory Medicine Nanfang Hospital Southern Medical University Guangzhou 510515 China

5. Nanozyme Medical Center Academy of Medical Science Zhengzhou University Zhengzhou 450001 China

6. Department of Pharmacy of Central China Fuwai Hospital Central China Fuwai Hospital of Zhengzhou University Zhengzhou 450001 China

Abstract

AbstractIntrinsic or acquired radioresistance remained an important challenge in the successful management of cancer. Herein, a novel “smart” multifunctional copper‐based nanocomposite (RCL@Pd@CuZ) to improve radiotherapy (RT) sensitivity is designed and developed. In this nanoplatform, DSPE‐PEG‐RGD modified on the liposome surface enhanced tumor targeting and permeability; capsaicin inserted into the phospholipid bilayer improved the hypoxic conditions in the tumor microenvironment (TME) by inhibiting mitochondrial respiration; a Cu MOF porous cube encapsulated in liposome generated highly active hydroxyl radicals (OH·), consumed GSH and promoted cuproptosis by releasing Cu2+; the ultrasmall palladium (Pd) nanozyme within the cubes exhibited peroxidase activity, catalyzing toxic OH· generation and releasing oxygen from hydrogen peroxide; and lastly, Pd, as an element with a relatively high atomic number (Z) enhanced the photoelectric and Compton effects of X‐rays. Therefore, RCL@Pd@CuZ enhance RT sensitivity by ameliorating hypoxia, promoting cuproptosis, depleting GSH, amplifying oxidative stress, and enhancing X‐ray absorption  , consequently potently magnifying immunogenic cell death (ICD). In a mouse model , RCL@Pd@CuZ combined with RT yielded >90% inhibition compared with that obtained by RT alone in addition to a greater quantity of DC maturation and CD8+ T cell infiltration. This nanoplatform offered a promising remedial modality to facilitate cuproptosis‐related cancer radioimmunotherapy.

Publisher

Wiley

Subject

Biomaterials,Biotechnology,General Materials Science,General Chemistry

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