Coordination Chemistry Based Approach to Lipophilic Inhibitors of 1-Deoxy-D-xylulose-5-phosphate Reductoisomerase

Deng LS; Sundriyal S; Rubio V; Shi ZZ; Song YC

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Coordination Chemistry Based Approach to Lipophilic Inhibitors of 1-Deoxy-D-xylulose-5-phosphate Reductoisomerase

机译：基于配位化学方法的1-脱氧-D-木酮糖-5-磷酸还原异构酶的亲脂性抑制剂

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摘要

1-Deoxy-D-xylulose-5-phosphate reductoisomerase (DXR) in the non-mevalonate pathway found in most bacteria is a validated anti-infective drug target. Fosmidomycin, a potent DXR inhibitor, is active against Gram-negative bacteria. A coordination chemistry and structure based approach was used to discover a novel, lipophilic DXR inhibitor with an IC50 of 1.4 mu M. It exhibited a broad spectrum of activity against Gram-negative and -positive bacteria with minimal inhibition concentrations of 20-100 mu M (or 3.7-19 mu g/mL).

机译：在大多数细菌中发现的非甲羟戊酸途径中的1-脱氧-D-木酮糖-5-磷酸还原异构酶（DXR）是经过验证的抗感染药物靶标。磷霉素（一种有效的DXR抑制剂）对革兰氏阴性细菌具有活性。基于配位化学和结构的方法用于发现新颖的亲脂性DXR抑制剂，IC50为1.4μM。它对革兰氏阴性和阳性细菌表现出广谱的活性，最小抑制浓度为20-100μM （或3.7-19μg / mL）。

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《Journal of Medicinal Chemistry》 |2009年第21期|共4页
作者
Deng LS; Sundriyal S; Rubio V; Shi ZZ; Song YC;
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正文语种 eng
中图分类药学;
关键词
SUBSTITUTED FOSMIDOMYCIN ANALOGS; 5-PHOSPHATE REDUCTOISOMERASE; MYCOBACTERIUM-TUBERCULOSIS; ISOPRENOID BIOSYNTHESIS; NONMEVALONATE PATHWAY; STABILITY-CONSTANTS; ANTIMALARIAL-DRUGS; ANTIBACTERIAL; ANTIBIOTICS; DERIVATIVES;

机译：替代性霜霉病模拟物;5-磷酸还原异构酶;结核分枝杆菌;异戊二烯生物合成;非甲羟戊酸途径;稳定性稳定;抗药性;抗菌;抗菌;

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1. Coordination Chemistry Based Approach to Lipophilic Inhibitors of 1-Deoxy-D-xylulose-5-phosphate Reductoisomerase [J] . Deng LS, Sundriyal S, Rubio V, Journal of Medicinal Chemistry . 2009,第21期

机译：基于配位化学方法的1-脱氧-D-木酮糖-5-磷酸还原异构酶的亲脂性抑制剂
2. Modifying lipophilicities of Zn(II) coordination species by introduction of ancillary ligands: A supramolecular chemistry approach [J] . Ma Z., Hopson R., Cai C., Crystal growth & design . 2010,第5期

机译：通过引入辅助配体来修饰Zn（II）配位物种的亲脂性：超分子化学方法
3. A structure-guided fragment-based approach for the discovery of allosteric inhibitors targeting the lipophilic binding site of transcription factor EthR [J] . Benoit Lechartier, Chris Abell, Nancy Ty, The biochemical journal . 2014,第2期

机译：基于结构指导的基于片段的方法，用于发现靶向转录因子EthR亲脂性结合位点的变构抑制剂
4. Design, Synthesis and Biological Activity of Ketol-acid Reductoisomerase Inhibitors [C] . Baolei Wang, Xinghai Liu, Yonghong Li, Proceedings of 4th international symposium on pesticides and environmental safety amp; 5th pan Pacific confernce on pesticide science amp; 8th international workshop on crop protection chemistry and regulatory harmonization . 2012

机译：酮酸还原异构酶抑制剂的设计，合成和生物活性
5. A coordination chemistry-based approach for the synthesis of stimulant-responsive supramolecular cofacial porphyrin complexes. [D] . Oliveri, Christopher Gordon. 2007

机译：基于配位化学的方法，用于合成兴奋剂反应性超分子界面卟啉配合物。
6. Structures of 1-Deoxy-D-Xylulose-5-Phosphate Reductoisomerase/Lipophilic Phosphonate Complexes [O] . Lisheng Deng, Kiwamu Endo, Masahiro Kato, 2011

机译：1-脱氧-D-木酮糖-5-磷酸还原异构酶/亲脂性膦酸酯复合物的结构
7. Molecular materials and devices: developing new functional systems based on the coordination chemistry approach [O] . Henrique E. Toma 2003

机译：分子材料和装置：基于协调化学方法开发新的功能系统

Coordination Chemistry Based Approach to Lipophilic Inhibitors of 1-Deoxy-D-xylulose-5-phosphate Reductoisomerase

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