紫杉醇
紫杉烷
癌症研究
药理学
癌细胞
下调和上调
生物
化学
乳腺癌
癌症
医学
内科学
生物化学
基因
作者
Dade Rong,Changwei Wang,Xiaomei Zhang,Yanli Wei,Mingming Zhang,Daiyuan Liu,Farhan Haider,Saleh Abdul Momen Ali,Yanbin Liu,Adam Taouil,Wanrong Guo,Yican Wang,Iwao Ojima,Shulan Yang,Haihe Wang
出处
期刊:Cancer Letters
[Elsevier BV]
日期:2020-07-27
卷期号:491: 36-49
被引量:14
标识
DOI:10.1016/j.canlet.2020.06.025
摘要
Paclitaxel (PTX) is widely used to treat breast and ovarian cancers, but innate and acquired resistance often compromises its applications. The objective of this study was to screen new-generation taxanes for their efficiency against both PTX-sensitive and PTX-resistant breast cancer cells. From twelve compounds, difluorovinyl-ortataxel (DFV-OTX) displayed potent cytotoxic activities against both PTX-sensitive and PTX-resistant breast cancer cells. Moreover, DFV-OTX effectively induced tubulin/microtubule polymerization and G2/M phase arrest, leading to apoptosis in both PTX-sensitive and PTX-resistant cancer cells. Molecular docking analysis showed that DFV-OTX possesses unique hydrogen-bonding and van der Waals interactions with β-tubulin. LC-MS/MS analysis also demonstrated that the intracellular drug amount of DFV-OTX was lower than that of PTX, which would be critical to overcome PTX-resistance. Furthermore, DFV-OTX exhibited clear efficacy in the MCF-7R and MDA-MB-231R tumor xenografts in mouse models. Taken together, our results demonstrate that the novel taxane, DFV-OTX, can effectively overcome PTX-resistance in MDA-MB-231R cells, wherein the drug resistance was attributed to ABCB1/ABCG2 upregulation and a distinct mode of action in MCF-7R cells. Our results strongly indicate that DFV-OTX is a promising chemotherapeutic agent for the treatment of PTX-resistant cancers. • DFV-OTX exhibited effective cytotoxicity against PTX-resistant breast cancer cells. • DFV-OTX had unique hydrogen-bonding and vdW interactions with β-tubulin. • DFV-OTX showed lower intracellular drug level but higher cytotoxicity than PTX. • DFV-OTX showed potent therapeutic efficacy against PTX-resistant tumor xenografts.
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