Trisulfide Bond‐Mediated Molecular Phototheranostic Platform for “Activatable” NIR‐II Imaging‐Guided Enhanced Gas/Chemo‐Hypothermal Photothermal Therapy

Author:

Wu Gui‐long1,Liu Fen1,Li Na1,Fu Qian1,Wang Cheng‐kun1,Yang Sha1,Xiao Hao1,Tang Li12,Wang Feirong1,Zhou Wei1,Wang Wenjie1,Kang Qiang1,Li Zelong1,Lin Nanyun1,Wu Yinyin1,Chen Guodong3,Tan Xiaofeng145,Yang Qinglai1345ORCID

Affiliation:

1. Center for Molecular Imaging Probe Hunan Province Key Laboratory of Tumor Cellular and Molecular Pathology Cancer Research Institute Hengyang Medical School University of South China Hengyang Hunan 421001 China

2. Key Laboratory of Tropical Medicinal Plant Chemistry of Ministry of Education College of Chemistry and Chemical Engineering Hainan Normal University Haikou Hainan 571158 China

3. Department of Hepatopancreatobiliary Surgery The First Affiliated Hospital Hengyang Medical School University of South China Hengyang Hunan 421001 China

4. National Health Commission Key Laboratory of Birth Defect Research and Prevention Hunan Provincial Maternal and Child Health Care Hospital Changsha Hunan 410008 China

5. MOE Key Lab of Rare Pediatric Diseases Hengyang Medical School University of South China Hengyang Hunan 421001 China

Abstract

AbstractTumor microenvironment (TME)‐triggered phototheranostic platform offers a feasible strategy to improve cancer diagnosis accuracy and minimize treatment side effects. Developing a stable and biocompatible molecular phototheranostic platform for TME‐activated second near‐infrared (NIR‐II) fluorescence imaging‐guided multimodal cascade therapy is a promising strategy for creating desirable anticancer agents. Herein, a new NIR‐II fluorescence imaging‐guided activatable molecular phototheranostic platform (IR‐FEP‐RGD‐S‐S‐S‐Fc) is presented for actively targeted tumor imaging and hydrogen sulfide (H2S) gas‐enhanced chemodynamic‐hypothermal photothermal combined therapy (CDT/HPTT). It is revealed for the first time that the coupling distance between IR‐FE and ferrocene is proportional to the photoinduced electron transfer (PET), and the aqueous environment is favorable for PET generation. The part of Cyclic‐RGDfK (cRGDfk) peptides can target the tumor and benefit the endocytosis of nanoparticles. The high‐concentration glutathione (GSH) in the TME will separate the fluorescence molecule and ferrocene by the GSH‐sensitive trisulfide bond, realizing light‐up NIR‐II fluorescence imaging and a cascade of trimodal synergistic CDT/HPTT/gas therapy (GT). In addition, the accumulation of hydroxyl radicals (•OH) and down‐regulation of glutathione peroxidase 4 (GPX4) can produce excessive harmful lipid hydroperoxides, ultimately leading to ferroptosis.

Funder

National Natural Science Foundation of China

Natural Science Foundation of Hunan Province

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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