Structure-Guided Design of Novel L-Cysteine Derivatives as Potent KSP Inhibitors

Ogo Naohisa; Ishikawa Yoshinobu; Sawada Jun-ichi; Matsuno Kenji; Hashimoto Akihiro; Asai Akira

首页> 外文期刊>ACS medicinal chemistry letters >Structure-Guided Design of Novel L-Cysteine Derivatives as Potent KSP Inhibitors

【24h】

Structure-Guided Design of Novel L-Cysteine Derivatives as Potent KSP Inhibitors

机译：新型L-半胱氨酸衍生物作为有效KSP抑制剂的结构导向设计

获取原文

获取原文并翻译 | 示例

掌桥外文数据库（机构版） >>

开具论文收录证明 >>

页面导航

摘要
著录项
相似文献
相关主题

摘要

Kinesin spindle protein (KSP), known as Hs Eg5, a member of the kinesin-5 family, plays an important role in the formation and maintenance of the bipolar spindle. We previously reported S-trityl-L-cysteine derivatives as selective KSP inhibitors. Here, we report further optimizations using docking modeling in the L5 allosteric binding site, which led to the discovery of several high affinity derivatives with two fused phenyl rings in the trityl group giving low nanomolar range KSP ATPase inhibition. The representative derivatives potently inhibited cell growth of HCT116 cells in correlation with KSP inhibitory activities and significantly suppressed tumor growth in the xenograft model in vivo.

机译：驱动蛋白纺锤体蛋白（KSP），称为Hs Eg5，是驱动蛋白5家族的成员，在双极纺锤体的形成和维持中起着重要作用。我们先前报道过S-三苯甲基-L-半胱氨酸衍生物作为选择性KSP抑制剂。在这里，我们报告了在L5变构结合位点使用对接模型的进一步优化，这导致了在三苯甲基中具有两个稠合苯环的几个高亲和力衍生物的发现，从而产生了低纳摩尔范围的KSP ATPase抑制作用。代表性衍生物在体内与KSP抑制活性相关地有效抑制HCT116细胞的细胞生长并显着抑制肿瘤生长。

著录项

来源
《ACS medicinal chemistry letters》 |2015年第9期|共6页
作者
Ogo Naohisa; Ishikawa Yoshinobu; Sawada Jun-ichi; Matsuno Kenji; Hashimoto Akihiro; Asai Akira;
展开▼
作者单位

展开▼
收录信息
原文格式 PDF
正文语种 eng
中图分类药学;化学;
关键词
Kinesin spindle protein; L-cysteine derivative; molecular modeling differential scanning fluorimetry; HCT-116 xenograft model;

机译：驱动蛋白纺锤体蛋白;L-半胱氨酸衍生物;分子模拟差示扫描荧光法;HCT-116异种移植模型;

相似文献

外文文献
中文文献
专利

1. Structure-Guided Design of Novel L-Cysteine Derivatives as Potent KSP Inhibitors [J] . Ogo Naohisa, Ishikawa Yoshinobu, Sawada Jun-ichi, ACS medicinal chemistry letters . 2015,第9期

机译：新型L-半胱氨酸衍生物作为有效KSP抑制剂的结构导向设计
2. Kinesin spindle protein (KSP) inhibitors. Part 8: Design and synthesis of 1,4-diaryl-4,5-dihydropyrazoles as potent inhibitors of the mitotic kinesin KSP. [J] . Roecker AJ, Coleman PJ, Mercer SP, Bioorganic and Medicinal Chemistry Letters . 2007,第20期

机译：驱动蛋白纺锤体蛋白（KSP）抑制剂。第8部分：设计和合成作为有丝分裂驱动蛋白KSP的有效抑制剂的1,4-二芳基-4,5-二氢吡唑。
3. Kinesin spindle protein (KSP) inhibitors. Part 7: Design and synthesis of 3,3-disubstituted dihydropyrazolobenzoxazines as potent inhibitors of the mitotic kinesin KSP. [J] . Garbaccio RM, Tasber ES, Neilson LA, Bioorganic and Medicinal Chemistry Letters . 2007,第20期

机译：驱动蛋白纺锤体蛋白（KSP）抑制剂。第7部分：设计和合成3,3-二取代的二氢吡唑并苯并恶嗪作为有丝分裂驱动蛋白KSP的有效抑制剂。
4. Molecular Docking Analysis of Podophyllotoxin Derivatives in Sulawesi Propolis as Potent Inhibitors of Protein Kinases [C] . Darin Flamandita, Kenny Lischer, Diah Kartika Pratami, International Symposium on Sustainable and Clean Energy;International Conference on Quality in Research . 2020

机译：洛叶葡萄球菌毒素衍生物的分子对接分析蛋白酶激酶有效抑制剂
5. Design, synthesis, and biological evaluation of betulinic acid derivatives as potent anti-HIV-1 agents. [D] . Qian, Keduo. 2008

机译：作为有效的抗HIV-1药物的桦木酸衍生物的设计，合成和生物学评估。
6. Structure-Guided Design of Novel l-Cysteine Derivatives as Potent KSP Inhibitors [O] . Naohisa Ogo, Yoshinobu Ishikawa, Jun-ichi Sawada, 2015

机译：新型l-半胱氨酸衍生物作为有效KSP抑制剂的结构导向设计
7. Structure-Guided Design of Novel l-Cysteine Derivatives as Potent KSP Inhibitors [O] . Naohisa Ogo, Yoshinobu Ishikawa, Jun-ichi Sawada, 2015

机译：新型L-半胱氨酸衍生物的结构引导设计为强效ksp抑制剂

Structure-Guided Design of Novel L-Cysteine Derivatives as Potent KSP Inhibitors

摘要

著录项

相似文献

相关主题

期刊订阅