紫杉醇
体内
生物相容性
线粒体
癌细胞
纳米颗粒
体外
化学
活性氧
纳米医学
纳米技术
生物物理学
材料科学
生物化学
癌症
生物
生物技术
有机化学
遗传学
作者
Xinjie Zhu,Ri‐Fei Li,Liang Xu,Hui Yin,Long Chen,Ye Yuan,Wu Zhong,Jian Lin
出处
期刊:Small
[Wiley]
日期:2018-11-19
卷期号:15 (2): e1803428-e1803428
被引量:27
标识
DOI:10.1002/smll.201803428
摘要
Self-assembled protein nanoparticles have attracted much attention in biomedicine because of their biocompatibility and biodegradability. Protein nanoparticles have become widely utilized as diagnostic or therapeutic agents for various cancers. However, there are no reports that protein nanoparticles can specifically target mitochondria. This targeting is desirable, since mitochondria are critical in the development of cancer cells. In this study, the discovery of a novel self-assembled metal protein nanoparticle, designated GST-MT-3, is reported, which targets the mitochondria of cancer cells within 30 min in vitro and rapidly accumulates in tumors within 1 h in vivo. The nanoparticles chelate cobalt ions [GST-MT-3(Co2+ )], which induces reactive oxygen species (ROS) production and reduces the mitochondrial membrane potential. These effects lead to antitumor activity in vivo. GST-MT-3(Co2+ ) with covalently conjugated paclitaxel synergistically suppress tumors and prolong survival. Importantly, the effective dosage of paclitaxel is 50-fold lower than that utilized in standard chemotherapy (0.2 vs 10 mg kg-1 ). To the best of the authors' knowledge, GST-MT-3 is the first reported protein nanoparticle that targets mitochondria. It has the potential to be an excellent platform for combination therapies.
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