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一种金属有机骨架(MOF)芬顿纳米试剂增强的纳米催化癌症治疗,与自噬抑制协同作用。

A Metal-Organic Framework (MOF) Fenton Nanoagent-Enabled Nanocatalytic Cancer Therapy in Synergy with Autophagy Inhibition.

机构信息

State Key Laboratory of High Performance Ceramics and Superfine Microstructure, Shanghai Institute of Ceramics, Chinese Academy of Sciences, Shanghai, 200050, P. R. China.

Center of Materials Science and Optoelectronics Engineering, University of Chinese Academy of Sciences, Beijing, 100049, P. R. China.

出版信息

Adv Mater. 2020 Mar;32(12):e1907152. doi: 10.1002/adma.201907152. Epub 2020 Feb 13.

Abstract

Nanocatalytic medicine has been developed recently to trigger intratumoral generation of highly toxic reactive oxygen species (ROS) for cancer therapy, which, unfortunately, suffers from compromised therapeutic efficacy due to a self-protective mechanism, autophagy, of cancer cells to mitigate oxidative damage. In this work, during the efforts of ROS generation by nanocatalytic medicine, a pharmacological autophagy inhibition strategy is implemented for augmenting ROS-induced oxidative damage for synergetic cancer therapy. An iron-containing metal-organic framework [MOF(Fe)] nanocatalyst as a peroxidase mimic is used to catalyze the generation of highly oxidizing •OH radicals specifically within cancer cells, while chloroquine is applied to deacidify lysosomes and inhibit autophagy, cutting off the self-protection pathway under severe oxidative stress. Cancer cells fail to extract their components to detoxicate and strengthen themselves, finally succumbing to the ROS-induced oxidative damage during nanocatalytic therapy. Both in vitro and in vivo results demonstrate the synergy between nanocatalytic therapy and autophagy inhibition, suggesting that such a combined strategy is applicable to amplify tumor-specific oxidative damage and may be informative to future design of therapeutic regimen.

摘要

纳米催化医学最近被开发出来,以触发肿瘤内产生高毒性活性氧(ROS)用于癌症治疗,但不幸的是,由于癌细胞的自保护机制自噬,会减轻氧化损伤,因此治疗效果受到影响。在这项工作中,在纳米催化药物产生 ROS 的过程中,实施了一种药理学自噬抑制策略,以增强 ROS 诱导的氧化损伤,从而实现协同癌症治疗。使用一种含有铁的金属-有机骨架[MOF(Fe)]纳米催化剂作为过氧化物酶模拟物,专门在癌细胞内催化生成强氧化性的•OH 自由基,而氯喹则用于降低溶酶体的酸度并抑制自噬,从而切断严重氧化应激下的自我保护途径。癌细胞无法提取其成分来解毒和增强自身,最终在纳米催化治疗过程中因 ROS 诱导的氧化损伤而死亡。体外和体内结果都证明了纳米催化治疗与自噬抑制之间的协同作用,表明这种联合策略可用于放大肿瘤特异性氧化损伤,可能为未来治疗方案的设计提供信息。

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