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首页> 美国卫生研究院文献>Acta Crystallographica Section F: Structural Biology and Crystallization Communications >Crystallization and initial crystallographic analysis of covalent DNA-cleavage complexes of Staphyloccocus aureus DNA gyrase with QPT-1 moxifloxacin and etoposide
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Crystallization and initial crystallographic analysis of covalent DNA-cleavage complexes of Staphyloccocus aureus DNA gyrase with QPT-1 moxifloxacin and etoposide

机译:金黄色葡萄球菌DNA促旋酶与QPT-1莫西沙星和依托泊苷共价DNA切割复合物的结晶和初步晶体学分析

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摘要

Fluoroquinolone drugs such as moxifloxacin kill bacteria by stabilizing the normally transient double-stranded DNA breaks created by bacterial type IIA topoisomerases. Previous crystal structures of Staphylococcus aureus DNA gyrase with asymmetric DNAs have had static disorder (with the DNA duplex observed in two orientations related by the pseudo-twofold axis of the complex). Here, 20-base-pair DNA homoduplexes were used to obtain crystals of covalent DNA-cleavage complexes of S. aureus DNA gyrase. Crystals with QPT-1, moxifloxacin or etoposide diffracted to between 2.45 and 3.15 Å resolution. A G/T mismatch introduced at the ends of the DNA duplexes facilitated the crystallization of slightly asymmetric complexes of the inherently flexible DNA-cleavage complexes.
机译:氟喹诺酮类药物(例如莫西沙星)通过稳定由细菌IIA型拓扑异构酶产生的通常短暂的双链DNA断裂来杀死细菌。以前带有不对称DNA的金黄色葡萄球菌DNA促旋酶的晶体结构具有静态紊乱(观察到DNA双链体在两个方向上都与复合物的假双倍轴有关)。在此,使用20个碱基对的DNA同源双链体获得金黄色葡萄球菌DNA促旋酶的共价DNA切割复合体的晶体。 QPT-1,莫西沙星或依托泊苷的晶体衍射至2.45至3.15Å分辨率。在DNA双链体末端引入的G / T错配促进了固有柔性DNA切割复合物的稍微不对称复合物的结晶。

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