Acceptor engineering produces ultrafast nonradiative decay in NIR-II Aza-BODIPY nanoparticles for efficient osteosarcoma photothermal therapy via concurrent apoptosis and pyroptosis

Zhenxiong Shi, Hua Bai, Jiaxing Wu, Xiaofei Miao, Jia Gao, Xianning Xu, Yi Liu, Jiamin Jiang, Jiaqi Yang, Jiaxin Zhang, Tao Shao, Bo Peng, Huili Ma, Dan Zhu, Guojing Chen, Wenbo Hu, Lin Li, Wei Huang

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38 引用 (Scopus)

摘要

Small-molecule photothermal agents (PTAs) with intense second near-infrared (NIR-II, 1,000 to 1,700 nm) absorption and high photothermal conversion efficiencies (PCEs) are promising candidates for treating deep-seated tumors such as osteosarcoma. To date, the development of small-molecule NIR-II PTAs has largely relied on fabricating donor acceptor donor (D A D/D∼) structures and limited success has been achieved. Herein, through acceptor engineering, a donor acceptor acceptor (D A A∼)-structured NIR-II aza-boron-dipyrromethene (aza-BODIPY) PTA (SW8) was readily developed for the 1,064-nm laser-mediated phototheranostic treatment of osteosarcoma. Changing the donor groups to acceptor groups produced remarkable red-shifts of absorption maximums from first near-infrared (NIR-I) regions (808 nm) to NIR-II ones (1,064 nm) for aza-BODIPYs (SW1 to SW8). Furthermore, SW8 self-Assembled into nanoparticles (SW8@NPs) with intense NIR-II absorption and an ultrahigh PCE (75%, 1,064 nm). This ultrahigh PCE primarily originated from an additional nonradiative decay pathway, which showed a 100-fold enhanced decay rate compared to that shown by conventional pathways such as internal conversion and vibrational relaxation. Eventually, SW8@NPs performed highly efficient 1,064-nm laser-mediated NIR-II photothermal therapy of osteosarcoma via concurrent apoptosis and pyroptosis. This work not only illustrates a remote approach for treating deep-seated tumors with high spatiotemporal control but also provides a new strategy for building high-performance small-molecule NIR-II PTAs.

源语言英语
文章编号0169
期刊Research
6
DOI
出版状态已出版 - 6月 2023

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