化学
微管蛋白
血管生成
体内
微管
细胞生长
细胞凋亡
细胞培养
体外
癌细胞
结构-活动关系
A549电池
生物化学
立体化学
药理学
癌症
癌症研究
细胞生物学
生物
遗传学
生物技术
作者
He Huang,Yongfang Yao,Guodong Hou,Cui Zhao,Jinling Qin,Yixin Zhang,Yongtao Duan,Chuanjun Song,Junbiao Chang
标识
DOI:10.1016/j.ejmech.2021.113708
摘要
We report the structural optimization of tanshinone IIA, a natural product which possesses anti-tumor properties but low water-solubility, weak antiproliferative activity and poor PK properties. A new series of ring A/C/D modified tanshinone analogues were synthesized and studied for their antiproliferative capacities against six human cancer cell lines. SAR study revealed that ring A cleavage of tanshinone IIA led to improved anti-cancer activity. Introduction of a methoxy group to the phenyl ring could enhance the anti-cancer activity even further. Compound 2f with methoxy group at C-8 position was selected as an early lead with IC50 values of 0.28-3.16 μM against six tested cell lines. 2f could bind to tubulin colchicine site, inhibit tubulin assembly and disrupt the normal formation of microtubule networks. Cellular mechanistic studies revealed that 2f induced apoptotic cell death of A549 cells in a dose-dependent manner. In vitro investigations showed that 2f impeded the tubule-formation of HUVECs and potently inhibited the proliferation, migration and invasion of A549 cells as well as HUVECs. Furthermore, the in vivo anti-angiogenic effect of 2f was confirmed via a zebrafish model test. The satisfactory physicochemical property and metabolic stability of 2f, as well as improved water-solubility, further suggested that 2f could serve as a promising tubulin inhibitor and anti-angiogenic agent.
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