基诺美
生物信息学
化学
体内
细胞生长
IC50型
体外
癌症研究
极光激酶
激酶
有丝分裂
细胞
癌症
细胞周期
基因
生物
生物化学
细胞生物学
遗传学
作者
Baowen Qi,Ling Zhong,Jun He,Hongjia Zhang,Fengqiong Li,Ting Wang,Jing Zou,Yao‐Xin Lin,Chengchen Zhang,Xiaoqiang Guo,Rui Li,Jianyou Shi
标识
DOI:10.1021/acs.jmedchem.9b00353
摘要
Aurora and polo-like kinases control the G2/M phase in cell mitosis, which are both considered as crucial targets for cancer cell proliferations. Here, naphthalene-based Aurora/PLK coinhibitors as leading compounds were designed through in silico approach, and a total of 36 derivatives were synthesized. One candidate (AAPK-25) was selected under in vitro cell based high throughput screening with an IC50 value = 0.4 μM to human colon cancer cell HCT-116. A kinome scan assay showed that AAPK-25 was remarkably selective to both Aurora and PLK families. The relevant genome pathways were also depicted by microarray based gene expression analysis. Furthermore, validated from a set of in vitro and in vivo studies, AAPK-25 significantly inhibited the development of the colon cancer growth and prolonged the median survival time at the end of the administration (p < 0.05). To sum up, AAPK-25 has a great potential to be developed for a chemotherapeutic agent in clinical use.
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