Backbone assignment of the N-terminal 24-kDa fragment of Escherichia coli topoisomerase IV ParE subunit

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Backbone assignment of the N-terminal 24-kDa fragment of Escherichia coli topoisomerase IV ParE subunit

机译：大肠杆菌拓扑异构酶IV ParE亚基N末端24 kDa片段的骨干分配

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Bacterial DNA topoisomerases are important drug targets due to their importance in DNA replication and low homology to human topoisomerases. The N-terminal 24 kDa region of E. coli topoisomerase IV E subunit (eParE) contains the ATP binding pocket. Structure-based drug discovery has been proven to be an efficient way to develop potent ATP competitive inhibitors against ParEs. NMR spectroscopy is a powerful tool to understand protein and inhibitor interactions in solution. In this study, we report the backbone assignment for the N-terminal domain of E. coli ParE. The secondary structural information and the assignment will aid in structure-based antibacterial agents development targeting eParE.

机译：细菌DNA拓扑异构酶由于其在DNA复制中的重要性以及与人拓扑异构酶的低同源性而成为重要的药物靶标。大肠杆菌拓扑异构酶IV E亚基（eParE）的N端24 kDa区域包含ATP结合袋。基于结构的药物发现已被证明是开发有效的针对ParE的ATP竞争性抑制剂的有效方法。 NMR光谱是了解溶液中蛋白质和抑制剂相互作用的有力工具。在这项研究中，我们报告了大肠杆菌ParE N末端域的骨干分配。二级结构信息和分配将有助于针对eParE的基于结构的抗菌剂开发。

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《Biomolecular NMR assignments》 |2016年第1期|共4页
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正文语种 eng
中图分类分子生物学;
关键词
NMR; Topoisomerase; Drug discovery; ParE; Resonance assignment;

机译：核磁共振;拓扑异构酶;药物发现;ParE;共振分配;

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1. Backbone assignment of the N-terminal 24-kDa fragment of Escherichia coli topoisomerase IV ParE subunit [J] . Biomolecular NMR assignments . 2016,第1期

机译：大肠杆菌拓扑异构酶IV ParE亚基N末端24 kDa片段的骨干分配
2. Letter to the Editor: Backbone resonance assignment of the N-terminal 24 kDa fragment of the gyrase B subunit from S-aureus complexed with novobiocin [J] . Klaus W., Gsell B., Senn H., Journal of Biomolecular NMR . 2000,第4期

机译：致编辑的信：与新生物素复合的S-金黄色葡萄球菌促旋酶B亚基的N端24 kDa片段的骨干共振分配
3. Backbone and side-chain H-1, C-13, and N-15 NMR assignments of the N-terminal domain of Escherichia coli LpoA [J] . Biomolecular NMR assignments . 2015,第1期

机译：大肠杆菌LpoA N末端结构域的骨架和侧链H-1，C-13和N-15 NMR分配
4. EXPRESSION OF RECOMBINANT NAD- INDEPENDENT FDH1 ALPHA SUBUNIT FROM METHYLOBACTERIUM EXTORQUENS AM1 IN ESCHERICHIA COLI AND REVERSIBLE INTERCONVERSION OF CARBON DIOXIDE AND FORMATE [C] . Hyojin Hwang American Chemical Society National Meeting Exhibition . 2014

机译：从甲基杆菌的重组NAD-无关的FDH1α亚基的表达在大肠杆菌中的甲基杆菌AM1和二氧化碳的可逆互联和甲酸
5. Physical and functional interaction between a bacterial condensin subunit MukB and topoisomerase IV in Escherichia coli. [D] . Hayama, Ryo. 2012

机译：细菌凝缩蛋白亚基MukB和拓扑异构酶IV在大肠杆菌中的物理和功能相互作用。
6. Crystal Structures of Escherichia coli Topoisomerase IV ParE Subunit (24 and 43 Kilodaltons): a Single Residue Dictates Differences in Novobiocin Potency against Topoisomerase IV and DNA Gyrase [O] . Steven Bellon, Jonathan D. Parsons, Yunyi Wei, 2004

机译：大肠杆菌拓扑异构酶IV ParE亚基（24和43 Kilodaltons）的晶体结构：单一的残留决定新霉素对拓扑异构酶IV和DNA促旋酶的功效的差异。
7. Crystal Structures of Escherichia coli Topoisomerase IV ParE Subunit (24 and 43 Kilodaltons): a Single Residue Dictates Differences in Novobiocin Potency against Topoisomerase IV and DNA Gyrase [O] . Bellon, Steven, Parsons, Jonathan D., Wei, Yunyi, 2004

机译：大肠杆菌拓扑异构酶IV ParE亚基（24和43 Kilodaltons）的晶体结构：单一的残留决定了新霉素对拓扑异构酶IV和DNA促旋酶效力的差异。

Backbone assignment of the N-terminal 24-kDa fragment of Escherichia coli topoisomerase IV ParE subunit

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