光动力疗法
谷胱甘肽
肺癌
光敏剂
活性氧
癌症研究
氧化应激
癌细胞
肺癌的治疗
化学
癌症
药理学
体内
医学
生物化学
生物
病理
内科学
光化学
酶
有机化学
生物技术
作者
Feiyi Sun,Yuyang Chen,Kristy W. K. Lam,Wutong Du,Qingqing Liu,Fei Han,Dan Li,Jacky W. Y. Lam,Jianwei Sun,Ryan T. K. Kwok,Ben Zhong Tang
出处
期刊:Small
[Wiley]
日期:2024-05-28
被引量:1
标识
DOI:10.1002/smll.202401334
摘要
Abstract Lung cancer, a highly prevalent and lethal form of cancer, is often associated with oxidative stress. Photodynamic therapy (PDT) has emerged as a promising alternative therapeutic tool in cancer treatments, but its efficacy is closely correlated to the photosensitizers generating reactive oxygen species (ROS) and the antioxidant capacity of tumor cells. In particular, glutathione (GSH) can reduce the ROS and thus compromise PDT efficacy. In this study, a GSH‐responsive near‐infrared photosensitizer (TBPPN) based on aggregation‐induced emission for real‐time monitoring of GSH levels and enhanced PDT for lung cancer treatment is developed. The strategic design of TBPPN, consisting of a donor–acceptor structure and incorporation of dinitrobenzene, enables dual functionality by not only the fluorescence being activated by GSH but also depleting GSH to enhance the cytotoxic effect of PDT. TBPPN demonstrates synergistic PDT efficacy in vitro against A549 lung cancer cells by specifically targeting different cellular compartments and depleting intracellular GSH. In vivo studies further confirm that TBPPN can effectively inhibit tumor growth in a mouse model with lung cancer, highlighting its potential as an integrated agent for the diagnosis and treatment of lung cancer. This approach enhances the effectiveness of PDT for lung cancer and deserves further exploration of its potential for clinical application.
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