Acrosin structure-based design, synthesis and biological activities of 7-azaindol derivatives as new acrosin inhibitors

引用本文: Jun Hang Jiang, Xue Fei Liu, Can Hui Zhen, You Jun Zhou, Ju Zhu, Jia Guo Lv, Chun Quan Sheng. Acrosin structure-based design, synthesis and biological activities of 7-azaindol derivatives as new acrosin inhibitors[J]. Chinese Chemical Letters, 2011, 22(3): 272-275. doi: 10.1016/j.cclet.2010.09.033 shu

Citation: Jun Hang Jiang, Xue Fei Liu, Can Hui Zhen, You Jun Zhou, Ju Zhu, Jia Guo Lv, Chun Quan Sheng. Acrosin structure-based design, synthesis and biological activities of 7-azaindol derivatives as new acrosin inhibitors[J]. Chinese Chemical Letters, 2011, 22(3): 272-275. doi: 10.1016/j.cclet.2010.09.033 shu

Acrosin structure-based design, synthesis and biological activities of 7-azaindol derivatives as new acrosin inhibitors

Department of Medicinal Chemistry, School of Pharmacy, Second Military Medical University, Shanghai 200433, China
基金项目:
This work was supported by the Shanghai Family Planning Commission Research Fund (No. 2007JG02) and Shanghai Leading Academic Discipline Project (No. B906).

摘要: A series of 7-azaindol derivatives were designed based on the homologous 3D model of human acrosin. These compounds were synthesized and evaluated for their human acrosin inhibitory activities in vitro. Compounds 7a, 7i, 7j, 7k and 7n showed highly inhibitory activity against human acrosin. The three-dimensional structure-activity relationship was investigated through a CoMFA model, which provided valuable information to further study of potential human acrosin inhibitors.

关键词:

Rational design
/ Azaindole
/ Synthesis
/ Acrosin
/ CoMFA

English

Acrosin structure-based design, synthesis and biological activities of 7-azaindol derivatives as new acrosin inhibitors

Department of Medicinal Chemistry, School of Pharmacy, Second Military Medical University, Shanghai 200433, China
Received Date: 08 June 2010
Fund Project:
This work was supported by the Shanghai Family Planning Commission Research Fund (No. 2007JG02) and Shanghai Leading Academic Discipline Project (No. B906).

Abstract: A series of 7-azaindol derivatives were designed based on the homologous 3D model of human acrosin. These compounds were synthesized and evaluated for their human acrosin inhibitory activities in vitro. Compounds 7a, 7i, 7j, 7k and 7n showed highly inhibitory activity against human acrosin. The three-dimensional structure-activity relationship was investigated through a CoMFA model, which provided valuable information to further study of potential human acrosin inhibitors.

Key words:

Rational design
/ Azaindole
/ Synthesis
/ Acrosin
/ CoMFA

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Acrosin structure-based design, synthesis and biological activities of 7-azaindol derivatives as new acrosin inhibitors

English

Acrosin structure-based design, synthesis and biological activities of 7-azaindol derivatives as new acrosin inhibitors

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通讯作者: 陈斌, bchen63@163.com

中国化学会秘书处

Acrosin structure-based design, synthesis and biological activities of 7-azaindol derivatives as new acrosin inhibitors

English

Acrosin structure-based design, synthesis and biological activities of 7-azaindol derivatives as new acrosin inhibitors

CCS Chemistry：嵌段共聚物自组装成 “三明治”二维有机材料，实现纳米级压力传感功能

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CCS Chemistry：工作高效不疲劳，只须让催化剂动起来

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CCS Chemistry：金黄色葡萄球菌醛基脱氢酶是如何识别特异性底物的？

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