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通过普鲁士蓝纳米药物产生碳自由基增强肿瘤光动力协同治疗效果。

Enhancing tumor photodynamic synergistic therapy efficacy through generation of carbon radicals by Prussian blue nanomedicine.

作者信息

Zhong Jun, Zhu Mingzhi, Guo Jiaqi, Chen Xinyu, Long Ruimin, Körte Fabian, Wang Shibin, Chen Hao, Xiong Xin, Liu Yuangang

机构信息

College of Chemical Engineering, Huaqiao University, Xiamen 361021, China.

NMI Natural and Medical Sciences Institute, University of Tübingen, Reutlingen 72770, Germany.

出版信息

Regen Biomater. 2024 Aug 24;11:rbae103. doi: 10.1093/rb/rbae103. eCollection 2024.

DOI:10.1093/rb/rbae103
PMID:39346686
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11434160/
Abstract

Significant progress has been achieved in tumor therapies utilizing nano-enzymes which could convert hydrogen peroxide into reactive oxygen species (ROS). However, the ROS generated by these enzymes possess a short half-life and exhibit limited diffusion within cells, making it challenging to inflict substantial damage on major organelles for effective tumor therapy. Therefore, it becomes crucial to develop a novel nanoplatform that could extend radicals half-life. Artesunate (ATS) is a Fe (II)-dependent drug, while the limited availability of iron (II), coupled with the poor aqueous solubility of ATS, limits its application. Here, Prussian blue (PB) was selected as a nano-carrier to release Fe (II), thus constructing a hollow Prussian blue/artesunate/methylene blue (HPB/ATS/MB) nanoplatform. HPB degraded and released iron(III), ATS and MB, under the combined effects of NIR irradiation and the unique tumor microenvironment. Moreover, Fe (III) exploited GSH to formation of Fe (II), disturbing the redox homeostasis of tumor cells and Fe (II) reacted with HO and ATS to generate carbon radicals with a long half-life . Furthermore, MB generates O under laser irradiation conditions. and experiments have demonstrated that the HPB/ATS/MB NPs exhibit a synergistic therapeutic effect through photothermal therapy, photodynamic therapy and radical therapy.

摘要

利用纳米酶将过氧化氢转化为活性氧(ROS)的肿瘤治疗已取得显著进展。然而,这些酶产生的ROS半衰期短,在细胞内的扩散有限,因此难以对主要细胞器造成实质性损伤以实现有效的肿瘤治疗。因此,开发一种能够延长自由基半衰期的新型纳米平台至关重要。青蒿琥酯(ATS)是一种依赖Fe(II)的药物,而Fe(II)的可用性有限以及ATS的水溶性差限制了其应用。在此,选择普鲁士蓝(PB)作为纳米载体来释放Fe(II),从而构建了一种中空普鲁士蓝/青蒿琥酯/亚甲蓝(HPB/ATS/MB)纳米平台。在近红外辐射和独特的肿瘤微环境的联合作用下,HPB降解并释放出铁(III)、ATS和MB。此外,Fe(III)利用谷胱甘肽形成Fe(II),扰乱肿瘤细胞的氧化还原稳态,并且Fe(II)与HO和ATS反应生成半衰期长的碳自由基。此外,MB在激光照射条件下产生单线态氧。体内和体外实验表明,HPB/ATS/MB纳米颗粒通过光热疗法、光动力疗法和自由基疗法表现出协同治疗效果。

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