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A study on quantitative structure–activity relationship and molecular docking of metalloproteinase inhibitors based on L-tyrosine scaffold

机译：基于L-酪氨酸支架的金属蛋白酶抑制剂的定量构效关系和分子对接研究

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BackgroundMMP-2 enzyme is a kind of matrix metalloproteinases that digests the denatured collagens and gelatins. It is highly involved in the process of tumor invasion and has been considered as a promising target for cancer therapy. The structural requirements of an MMP-2 inhibitor are: (1) a functional group that binds the zinc ion, and (2) a functional group which interacts with the enzyme backbone and the side chains which undergo effective interactions with the enzyme subsites.

机译：背景MMP-2酶是一种基质金属蛋白酶，可消化变性的胶原蛋白和明胶。它高度参与肿瘤的侵袭过程，并被认为是癌症治疗的有希望的靶标。 MMP-2抑制剂的结构要求是：（1）结合锌离子的官能团，和（2）与酶主链和与酶亚位点进行有效相互作用的侧链相互作用的官能团。

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期刊名称 DARU Journal of Pharmaceutical Sciences
作者
Maryam Abbasi; Fatemeh Ramezani; Maryam Elyasi; Hojjat Sadeghi-Aliabadi; Massoud Amanlou;
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作者单位

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年(卷),期 2015(23),1
年度 2015
页码 29
总页数 10
原文格式 PDF
正文语种
中图分类药学;
关键词
GA-PLS Metalloproteinase inhibitors MLR Molecular docking QSAR;

机译：GA-PLS;金属蛋白酶抑制剂;MLR;分子对接;QSAR;

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专利

1. A study on quantitative structure–activity relationship and molecular docking of metalloproteinase inhibitors based on L-tyrosine scaffold [J] . Maryam Abbasi, Fatemeh Ramezani, Maryam Elyasi, Daru Journal of pharmaceutical sciences. . 2015,第1期

机译：基于L-酪氨酸支架的金属蛋白酶抑制剂的定量构效关系和分子对接研究
2. CoMFA/CoMSIA and Molecular Docking Studies of Novel Matrix Metalloproteinase-2 Inhibitors Based on L-tyrosine Scaffold [J] . Jun-Zhang, Wang Xue-Jiao, Dong Zhen-Ke, Letters in drug design & discovery . 2016,第5期

机译：CoMFA / CoMSIA和基于L-酪氨酸支架的新型基质金属蛋白酶2抑制剂的分子对接研究
3. The Discovery of Novel Histone Lysine Methyltransferase G9a Inhibitors (Part 1): Molecular Design Based on a Series of Substituted 2,4-Diamino-7-aminoalkoxyquinazoline by Molecular-Docking-Guided 3D Quantitative Structure-Activity Relationship Studies [J] . Feng Taotao, Wang Hai, Zhang Xiaojin, Medicinal chemistry . 2014,第4期

机译：新型组蛋白赖氨酸甲基转移酶G9a抑制剂的发现（第1部分）：通过一系列分子对接的3D定量结构与活性关系研究，基于一系列取代的2,4-二氨基-7-氨基烷氧基喹唑啉的分子设计
4. Quantitative Structure-Activity Relationships for Phenyl Triazolinones of Protoporphyrinogen Oxidase Inhibitors: A Density Functional Theory Study [C] . JIAN WAN, LI ZHANG, GUANGFU YANG 第二届全国分子模拟与信息技术软件应用研讨会暨第四届创腾科技用户大会 . 2005

机译：原卟啉原氧化酶抑制剂的苯基三唑啉酮的定量构效关系：密度泛函理论研究
5. In silico screening for novel inhibitors of human neutrophil elastase using an integrated approach of quantitative structure activity relationship modeling and protein-ligand docking. [D] . Nguyen, Christian V. 2014

机译：在计算机上使用定量结构活性关系建模和蛋白质-配体对接的集成方法筛选人类嗜中性粒细胞弹性蛋白酶的新型抑制剂。
6. Quantitative structure-activity relationship and molecular docking studies of a series of quinazolinonyl analogues as inhibitors of gamma amino butyric acid aminotransferase [O] . Usman Abdulfatai, Adamu Uzairu, Sani Uba 2017

机译：一系列喹唑啉酮类似物作为γ-氨基丁酸氨基转移酶抑制剂的定量构效关系和分子对接研究
7. A study on quantitative structure–activity relationship and molecular docking of metalloproteinase inhibitors based on L-tyrosine scaffold [O] . Maryam Abbasi, Fatemeh Ramezani, Maryam Elyasi, 2015

机译：基于L-酪氨酸支架的金属蛋白酶抑制剂的定量构效关系和分子对接研究
8. Quantitative Structure-Activity Relationships of Beta-Adrenergic Agents. Application of the Computer Automated Structure Evaluation (CASE) Technique of Molecular Fragment Recognition [R] . Klopman, G., Kalos, A. N. 1986

机译：β-肾上腺素能药物的定量构效关系。分子片段识别计算机自动结构评估（CasE）技术的应用

A study on quantitative structure–activity relationship and molecular docking of metalloproteinase inhibitors based on L-tyrosine scaffold

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