紫杉醇
纳米载体
纳米笼
体内
细胞毒性
药物输送
内吞作用
流式细胞术
体外
药理学
材料科学
化学
生物物理学
纳米技术
细胞
癌症
生物化学
分子生物学
医学
生物
催化作用
生物技术
内科学
作者
Ruike Li,Yuanmeng Ma,Yixin Dong,Zhihui Zhao,Chaoqun You,Shenlin Huang,Xun Li,Fei Wang,Yu Zhang
出处
期刊:ACS Biomaterials Science & Engineering
[American Chemical Society]
日期:2019-11-13
卷期号:5 (12): 6645-6654
被引量:26
标识
DOI:10.1021/acsbiomaterials.9b01533
摘要
Paclitaxel (PTX), an excellent chemotherapeutic antitumor drug, is widely used to treat patients with various cancers. However, its clinical applications are greatly restricted by poor solubility and lack of targeting. Herein, we applied natural human H chain ferritin (HFtn) nanocages that can bind to tumor cells via interacting with the human transferritin receptor 1 (TfR1) leading to its endocytosis as the PTX carrier for the targeted delivery. PTX molecules were encapsulated into HFtn cavity using disassembly/reassembly method through adjusting pH. According to the requirements of drugs suitable for clinical trials, HFtn can be easily purified in high yields with no ligand modification or property modulation. We demonstrated that PTX molecules were successfully encapsulated in the protein nanocages. The HFtn-PTX nanoparticles exhibited similar morphology and structural characteristics to the hollow cage and showed significant cytotoxicity in vitro than the naked PTX. Flow cytometry, confocal laser scanning microscopy, and in vivo imaging of MDA-MB-231 tumor demonstrated the HFtn-PTX nanoparticles targeting ability to tumor cells. Cell apoptosis assay showed that HFtn-PTX had similar apoptotic characteristics on MDA-MB-231 cells as that of the free PTX. HFtn-PTX nanoparticles have higher in vivo therapeutic efficacy and lower systemic toxicity. The BALB/c mice model also confirmed the effectiveness of the nanoparticles. Specifically targeting to tumors and solving the solubility issue of water-insoluble drugs thus alleviating the side effects, HFtn can be an efficient hydrophobic drug delivery nanocarrier for further applications in cancer therapy.
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