National Institute of Cancer Research, National Health Research Institutes, Miaoli 35053, Taiwan.
Department of Nursing, National Quemoy University, Kinmen 89250, Taiwan.
EBioMedicine. 2018 Oct;36:241-251. doi: 10.1016/j.ebiom.2018.09.030. Epub 2018 Oct 5.
Cdc7-Dbf4 is a conserved serine/threonine kinase that plays an important role in initiation of DNA replication and DNA damage tolerance in eukaryotic cells. Cdc7 has been found overexpressed in human cancer cell lines and tumor tissues, and the knockdown of Cdc7 expression causes an p53-independent apoptosis, suggesting that Cdc7 is a target for cancer therapy. Only a handful Cdc7 kinase inhibitors have been reported. All Cdc7 kinase inhibitors, including PHA-767491, were identified and characterized as ATP-competitive inhibitors. Unfortunately, these ATP-competitive Cdc7 inhibitors have no good effect on clinical trial.
Here, we have developed a novel drug-screening platform to interrupt the interaction between Cdc7 and Dbf4 based on Renilla reniformis luciferase (Rluc)-linked protein-fragment complementation assay (Rluc-PCA). Using drug repositioning approach, we found several promising Cdc7 inhibitors for cancer therapy from a FDA-approved drug library.
Our data showed that dequalinium chloride and clofoctol we screened inhibit S phase progression, accumulation in G2/M phase, and Cdc7 kinase activity. In addition, in vivo mice animal study suggests that dequalinium chloride has a promising anti-tumor activity in oral cancer. Interestingly, we also found that dequalinium chloride and clofoctol sensitize the effect of platinum compounds and radiation due to synergistic effect. In conclusion, we identified non-ATP-competitive Cdc7 kinase inhibitors that not only blocks DNA synthesis at the beginning but also sensitizes cancer cells to DNA damage agents.
The inhibitors will be a promising anti-cancer agent and enhance the therapeutic effect of chemotherapy and radiation for current cancer therapy. FUND: This work was supported by grants from the Ministry of Science and Technology, Ministry of Health and Welfare, and National Health Research Institutes, Taiwan.
Cdc7-Dbf4 是一种保守的丝氨酸/苏氨酸激酶,在真核细胞的 DNA 复制起始和 DNA 损伤耐受中发挥重要作用。Cdc7 在人类癌细胞系和肿瘤组织中表达过度,Cdc7 表达的敲低会导致 p53 非依赖性细胞凋亡,表明 Cdc7 是癌症治疗的靶点。目前仅报道了少数几种 Cdc7 激酶抑制剂。所有 Cdc7 激酶抑制剂,包括 PHA-767491,均被鉴定为 ATP 竞争性抑制剂。不幸的是,这些 ATP 竞争性 Cdc7 抑制剂在临床试验中效果不佳。
在这里,我们开发了一种基于海肾荧光素酶(Rluc)连接的蛋白片段互补测定(Rluc-PCA)的新型药物筛选平台,以干扰 Cdc7 和 Dbf4 之间的相互作用。我们使用药物再定位方法,从 FDA 批准的药物库中发现了几种有希望用于癌症治疗的 Cdc7 抑制剂。
我们的数据表明,筛选出的地喹氯铵和氯己定抑制 S 期进展、G2/M 期积累和 Cdc7 激酶活性。此外,体内小鼠动物研究表明,地喹氯铵在口腔癌中有很好的抗肿瘤活性。有趣的是,我们还发现地喹氯铵和氯己定由于协同作用而增强了铂类化合物和辐射的效果。总之,我们鉴定出了非 ATP 竞争性 Cdc7 激酶抑制剂,不仅能在起始阶段阻断 DNA 合成,还能使癌细胞对 DNA 损伤剂敏感。
这些抑制剂将是一种很有前途的抗癌药物,并增强当前癌症治疗中化疗和放疗的治疗效果。
本工作得到了科技部、卫生福利部和国家卫生研究院的资助。
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