| Literature DB >> 30778211 |
Ningqiang Gong1,2,3, Xiaowei Ma1, Xiaoxia Ye1, Qunfang Zhou4, Xiaoai Chen1, Xiaoli Tan5, Shengkun Yao6, Shuaidong Huo1, Tingbin Zhang1, Shizhu Chen1,7, Xucong Teng2, Xixue Hu1, Jie Yu4, Yaling Gan1, Huaidong Jiang6, Jinghong Li8, Xing-Jie Liang9,10.
Abstract
Mitochondrial redox homeostasis, the balance between reactive oxygen species and antioxidants such as glutathione, plays critical roles in many biological processes, including biosynthesis and apoptosis, and thus is a potential target for cancer treatment. Here, we report a mitochondrial oxidative stress amplifier, MitoCAT-g, which consists of carbon-dot-supported atomically dispersed gold (CAT-g) with further surface modifications of triphenylphosphine and cinnamaldehyde. We find that the MitoCAT-g particles specifically target mitochondria and deplete mitochondrial glutathione with atomic economy, thus amplifying the reactive oxygen species damage caused by cinnamaldehyde and finally leading to apoptosis in cancer cells. We show that imaging-guided interventional injection of these particles potently inhibits tumour growth in subcutaneous and orthotopic patient-derived xenograft hepatocellular carcinoma models without adverse effects. Our study demonstrates that MitoCAT-g amplifies the oxidative stress in mitochondria and suppresses tumour growth in vivo, representing a promising agent for anticancer applications.Entities:
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Year: 2019 PMID: 30778211 DOI: 10.1038/s41565-019-0373-6
Source DB: PubMed Journal: Nat Nanotechnol ISSN: 1748-3387 Impact factor: 39.213