Molecular docking studies on oxidosqualene cyclase with 4-piperidinopyridine and 4-piperidinopyrimidine as its inhibitors

G. Jhansi Rani; M. Vinoth; P. Anitha

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Molecular docking studies on oxidosqualene cyclase with 4-piperidinopyridine and 4-piperidinopyrimidine as its inhibitors

机译：以4-哌啶子吡啶和4-哌啶子嘧啶为抑制剂的氧化角鲨烯环化酶的分子对接研究

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Oxidosqualene cyclase (OSC) or Lanostrol Synthase is one of the major enzyme in cholesterol biosynthesis. OSC is involved in conversion of squalene to lanosterol. Increased level of cholesterol in blood leads to hypercholesterolemia and major risk factor for cardiovascular diseases. Statin drug molecule is developed to inhibit HMGCoA, which is the first enzyme of cholesterol biosynthesis showed major side effects. Insilico predictions based on the crystal structure of OSC are performed. Active molecular docking studies using GOLD software reveals 4-piperidinopyridine and 4-piperidinopyrimidine (piperidino derivatives) are potent inhibitors of OSC and satisfy ADME properties. The PASS (Prediction of Activity Spectra for Substances) prediction results show the inhibiting activity of OSC enzyme.

机译：氧化角鲨烯环化酶（OSC）或Lanostrol合酶是胆固醇生物合成中的主要酶之一。 OSC参与了角鲨烯向羊毛甾醇的转化。血液中胆固醇水平的升高会导致高胆固醇血症和心血管疾病的主要危险因素。他汀类药物分子被开发来抑制HMGCoA，这是胆固醇生物合成中显示出主要副作用的第一种酶。执行基于OSC晶体结构的硅片预测。使用GOLD软件进行的主动分子对接研究表明4-piperidinopyridine和4-piperidinopyrimidine（piperidino衍生物）是OSC的有效抑制剂，并满足ADME特性。 PASS（物质活性谱的预测）预测结果显示了OSC酶的抑制活性。

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《Journal of Bioinformatics and Sequence Analysis》 |2011年第3期|共6页
作者
G. Jhansi Rani; M. Vinoth; P. Anitha;
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中图分类生物工程学（生物技术）;
关键词
Oxidosqualene cyclase (OSC)piperidino derivativesmolecular dockingtoxicity testingprediction of activity spectra for substances (PASS);

机译：氧化角鲨烯环化酶（OSC）哌啶子基衍生物分子对接毒性测试物质活性谱的预测（PASS）;

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1. A novel series of 4-piperidinopyridine and 4-piperidinopyrimidine inhibitors of 2,3-oxidosqualene cyclase-lanosterol synthase. [J] . Brown GR, strazeneca.com, Hollinshead DM, Journal of Medicinal Chemistry . 2000,第26期

机译：2,3-氧化角鲨烯环化酶-羊毛甾醇合酶的4-哌啶基吡啶和4-哌啶基嘧啶的新型抑制剂系列。
2. Novel 4-piperidinopyridine inhibitors of oxidosqualene cyclase-lanosterol synthase derived by consideration of inhibitor pK(a). [J] . Brown GR, strazeneca.com, Foubister AJ, Bioorganic and Medicinal Chemistry Letters . 2001,第16期

机译：考虑抑制剂pK（a）衍生的新型氧化氧角鲨烯环化酶-羊毛甾醇合酶的4-哌啶子吡啶抑制剂。
3. Synthesis and Structure-Activity Studies of Novel Orally Active Non-Terpenoic 2,3-Oxidosqualene Cyclase Inhibitors [J] . Henrietta Dehmlow, Johannes D. Aebi, Synese Jolidon, Journal of Medicinal Chemistry . 2003,第15期

机译：新型口服活性非萜2,3-氧代角鲨烯环化酶抑制剂的合成及结构活性研究
4. Study of Molecular Mechanism between 5-Lipoxygenase and Inhibitor in Comparison with Its Natural Substrate by Molecular Docking [C] . Kulpavee Jitapunkul, Pisanu Toochinda, Luckhana Lawtrakul Asian Conference on Defence Technology . 2016

机译：用分子对接与其天然底物相比的5-脂氧合酶和抑制剂的分子机制研究
5. Combination of the Computational Methods: Molecular dynamics, Homology Modeling and Docking to Design Novel Inhibitors and Study Structural Changes in Target Proteins for Current Diseases. [D] . Parra, Katherine. 2014

机译：计算方法的组合：分子动力学，同源性建模和对接，以设计新型抑制剂并研究当前疾病靶蛋白的结构变化。
6. Molecular Docking and Molecular Dynamics Studies on Selective Synthesis of α-Amyrin and β-Amyrin by Oxidosqualene Cyclases from Ilex Asprella [O] . Zhixue Wu, Hui Xu, Meiling Wang, 2019

机译：Ilex Asprella的氧化角鲨烯环化酶选择性合成α-Amyrin和β-Amyrin的分子对接和分子动力学研究
7. Homology modeling and docking studies on oxidosqualene cyclases associated with primary and secondary metabolism of Centella asiatica [O] . Vadlapudi Kumar, Chethan S Kumar, Gajula Hari, 2013

机译：与积雪草初次和二次代谢相关的氧化角鲨烯环化酶的同源性建模和对接研究

Molecular docking studies on oxidosqualene cyclase with 4-piperidinopyridine and 4-piperidinopyrimidine as its inhibitors

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