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Identification of Novel Cdc7 Kinase Inhibitors as Anti-Cancer Agents that Target the Interaction with Dbf4 by the Fragment Complementation and Drug Repositioning Approach

机译：鉴定新型Cdc7激酶抑制剂作为抗癌剂其通过片段互补和药物重新定位方法靶向与Dbf4的相互作用

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摘要

BackgroundCdc7-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.

机译：背景Cdc7-Dbf4是一种保守的丝氨酸/苏氨酸激酶，在真核细胞中启动DNA复制和DNA损伤耐受性中起重要作用。已经发现Cdc7在人类癌细胞系和肿瘤组织中过表达，而敲除Cdc7的表达会导致p53独立的细胞凋亡，这表明Cdc7是癌症治疗的靶标。仅报道了少数Cdc7激酶抑制剂。包括PHA-767491在内的所有Cdc7激酶抑制剂均被鉴定为ATP竞争性抑制剂。不幸的是，这些具有ATP竞争能力的Cdc7抑制剂在临床试验中没有良好的效果。

著录项

期刊名称 EBioMedicine
作者
An Ning Cheng; Yu-Kang Lo; Yi-Sheng Lin; Tswen-Kei Tang; Chun-Hua Hsu; John T.-A. Hsu; Alan Yueh-Luen Lee;
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作者单位

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年(卷),期 2018(36),-1
年度 2018
页码 241–251
总页数 11
原文格式 PDF
正文语种
中图分类
关键词
Cdc7 inhibitor Drug repositioning Cancer therapy Protein fragment complementation assay Protein-protein interaction;

机译：Cdc7抑制剂;药物重新定位;癌症治疗;蛋白质片段互补分析;蛋白质-蛋白质相互作用;

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专利

1. Identification of Novel Cdc7 Kinase Inhibitors as Anti-Cancer Agents that Target the Interaction with Dbf4 by the Fragment Complementation and Drug Repositioning Approach [J] . An Ning Cheng, Yu-Kang Lo, Yi-Sheng Lin, EBioMedicine . 2018,第152期

机译：鉴定新型Cdc7激酶抑制剂作为抗癌剂，其通过片段互补和药物重新定位方法靶向与Dbf4的相互作用
2. Budding yeast Dbf4 sequences required for Cdc7 kinase activation and identification of a functional relationship between the Dbf4 and Rev1 BRCT domains. [J] . Harkins V, Gabrielse C, Haste Genetics: A Periodical Record of Investigations Bearing on Heredity and Variation . 2009,第4期

机译：Cdc7激酶激活所需的萌芽酵母Dbf4序列，以及Dbf4和Rev1 BRCT域之间功能关系的鉴定。
3. Budding Yeast Dbf4 Sequences Required for Cdc7 Kinase Activation and Identification of a Functional Relationship Between the Dbf4 and Rev1 BRCT Domains [J] . Carrie Gabrielse, Louise Haste, Michael Weinreich, Genetics: A Periodical Record of Investigations Bearing on Heredity and Variation . 2009,第4期

机译：Cdc7激酶激活所需的芽酵母Dbf4序列以及Dbf4和Rev1 BRCT域之间功能关系的鉴定
4. A Network Integration Approach for Drug-Target Interaction Prediction and Computational Drug Repositioning from Heterogeneous Information [C] . Yunan Luo, Xinbin Zhao, Jingtian Zhou, Annual international conference on research in computational molecular biology . 2017

机译：一种基于异构信息的药物-目标相互作用预测和计算药物重新定位的网络集成方法
5. Novel Anti-Cancer Agents Targeting Epidermal Growth Factor (EGF) Protein-Protein Interactions [D] . Yawson, Emmanuel. 2019

机译：靶向表皮生长因子（EGF）蛋白质 - 蛋白质相互作用的新型抗癌剂
6. Budding Yeast Dbf4 Sequences Required for Cdc7 Kinase Activation and Identification of a Functional Relationship Between the Dbf4 and Rev1 BRCT Domains [O] . Victoria Harkins, Carrie Gabrielse, Louise Haste, 2009

机译：Cdc7激酶激活所需的芽酵母Dbf4序列以及Dbf4和Rev1 BRCT域之间功能关系的鉴定
7. Identification of Novel Cdc7 Kinase Inhibitors as Anti-Cancer Agents that Target the Interaction with Dbf4 by the Fragment Complementation and Drug Repositioning Approach [O] . An Ning Cheng, Yu-Kang Lo, Yi-Sheng Lin, 2018

机译：用片段互补和药物排雷方法鉴定新的CDC7激酶抑制剂作为抗癌试剂，其靶向与DBF4的相互作用和药物排雷方法

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