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ABCB1 structural models, molecular docking, and synthesis of new oxadiazolothiazin-3-one inhibitors

机译：ABCB1的结构模型，分子对接和新型恶二唑并噻嗪-3-酮抑制剂的合成

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Docking methods are powerful tools for in silico screening and drug lead generation and optimization. Here, we describe the synthesis of new inhibitors of ABCB1 whose design was based on construction and preliminary confirmation of a model for this membrane transporter of the ATP-binding cassette family. We chose the strategy to build our three-dimensional model of the ABCB1 transporter by homology. Atomic coordinates were then assayed for their reliability using the measured activity of some oxadiazolothiazin-3-one compounds. Once established their performance by docking analysis, we synthesized new compounds whose forecasted activity was tested by MTT and cytofluorimetric assays. Our docking model of MDR1, MONBD1, seems to reliably satisfy our need to design and forecast, on the basis of their LTCC blockers ability, the inhibitory activity of new molecules on the ABCB1 transporter

机译：对接方法是用于计算机筛选以及药物线索生成和优化的强大工具。在这里，我们描述了新的ABCB1抑制剂的合成，其设计基于对ATP结合盒家族膜转运蛋白的构建和模型的初步确认。我们选择了通过同源性构建ABCB1转运蛋白三维模型的策略。然后，使用一些恶二唑并噻嗪-3-酮化合物的活性，分析原子坐标的可靠性。通过对接分析确定其性能后，我们合成了新化合物，其预测活性已通过MTT和细胞荧光测定法进行了测试。我们的MDR1对接模型MONBD1似乎可以可靠地满足我们对LTCC阻断剂的设计和预测需求，即新分子对ABCB1转运蛋白的抑制活性

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C. Rosano; M. Viale; B. Cosimelli; E. Severi; R. Gangemi; A. Ciogli; D. De Totero; D. Spinelli;
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年度 2013
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1. ABCB1 Structural Models, Molecular Docking, and Synthesis of New Oxadiazolothiazin-3-one Inhibitors [J] . Camillo Rosano, Maurizio Viale, Barbara Cosimelli ACS medicinal chemistry letters . 2013,第8期

机译：ABCB1结构模型，分子对接和新的Oxadiazolothiazin-3-one抑制剂的合成。
2. Identification of Novel Structurally Diverse Anaplastic Lymphoma Kinase Inhibitors Based on Pharmacophore Modeling, Virtual Screening and Molecular Docking [J] . You Rong, Zhou Lu, Zhong Liangliang, Combinatorial chemistry & high throughput screening . 2016,第9期

机译：基于药物模拟，虚拟筛选和分子对接的新型结构多样性促进淋巴瘤激酶抑制剂
3. Molecular Docking Guided Comparative GFA, G/PLS, SVM and ANN Models of Structurally Diverse Dual Binding Site Acetylcholinesterase Inhibitors [J] . Shikhar Gupta, Adyary Fallarero, Mikko J. Vainio, Molecular informatics . 2011,第8期

机译：分子对接指导的结构多样的双结合位点乙酰胆碱酯酶抑制剂的比较GFA，G / PLS，SVM和ANN模型
4. Synthesis, In Silico Molecular Docking Modeling and Pharmacophore Mapping of (E)-3-(4-Hydroxy-2,6-Dimethoxyphenyl)-1 -Phenylprop-2-en-1 - One as Potential New Inhibitor of Microsomal Prostaglandin E2 Synthase-1 [C] . Pitipat Sanphetchaloemchok, Mohd Fadhlizil Fasihi Mohd Aluwi, Kamal Rullah, Postgraduate Symposium on Industrial Science and Technology . 2020

机译：（E）-3-（4-羟基-2,6-二甲氧基苯基）-1-phenylprop-2-en-1的硅分子对接建模和药效线映射，作为微粒体前列腺素E2合酶的潜在新抑制剂 - 1
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. ABCB1 Structural Models Molecular Docking and Synthesisof New Oxadiazolothiazin-3-one Inhibitors [O] . Camillo Rosano, Maurizio Viale, *, 2013

机译：ABCB1结构模型分子对接和合成种新型Oxadiazolothiazin-3-one抑制剂的制备
7. ABCB1 Structural Models, Molecular Docking, and Synthesis of New Oxadiazolothiazin-3-one Inhibitors [O] . C. Rosano, M. Viale, B. Cosimelli, 2013

机译：aBCB1结构模型，分子对接和新的合成恶二唑噻嗪-3-酮抑制剂

ABCB1 structural models, molecular docking, and synthesis of new oxadiazolothiazin-3-one inhibitors

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