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首页> 外文期刊>Journal of Molecular Biology >A new crystal structure of the bifunctional antibiotic simocyclinone D8 bound to DNA gyrase gives fresh insight into the mechanism of inhibition
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A new crystal structure of the bifunctional antibiotic simocyclinone D8 bound to DNA gyrase gives fresh insight into the mechanism of inhibition

机译:与DNA旋转酶结合的双功能抗生素simocyclinone D8的新晶体结构提供了新的抑制机制

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摘要

Simocyclinone D8 (SD8) is an antibiotic produced by Streptomyces antibioticus that targets DNA gyrase. A previous structure of SD8 complexed with the N-terminal domain of the DNA gyrase A protein (GyrA) suggested that four SD8 molecules stabilized a tetramer of the protein; subsequent mass spectrometry experiments suggested that a protein dimer with two symmetry-related SD8s was more likely. This work describes the structures of a further truncated form of the GyrA N-terminal domain fragment with and without SD8 bound. The structure with SD8 has the two SD8 molecules bound within the same GyrA dimer. This new structure is entirely consistent with the mutations in GyrA that confer SD8 resistance and, by comparison with a new apo structure of the GyrA N-terminal domain, reveals the likely conformation changes that occur upon SD8 binding and the detailed mechanism of SD8 inhibition of gyrase. Isothermal titration calorimetry experiments are consistent with the crystallography results and further suggest that a previously observed complex between SD8 and GyrB is ~ 1000-fold weaker than the interaction with GyrA.
机译:Simocyclinone D8(SD8)是由链霉菌产生的一种靶向DNA促旋酶的抗生素。与DNA旋转酶A蛋白(GyrA)的N端结构域复合的SD8先前结构表明,四个SD8分子稳定了该蛋白的四聚体。随后的质谱实验表明,具有两个与对称相关的SD8s的蛋白二聚体的可能性更大。这项工作描述了具有和不具有SD8结合的GyrA N末端域片段的进一步截短形式的结构。 SD8的结构使两个SD8分子结合在同一个GyrA二聚体中。这种新结构与赋予SD8抗性的GyrA突变完全一致,并且与GyrA N末端域的新载脂蛋白结构相比,揭示了SD8结合后可能发生的构象变化以及SD8抑制SD8的详细机制。旋转酶。等温滴定量热法实验与晶体学结果一致,并进一步表明,先前观察到的SD8和GyrB之间的复合物比与GyrA的相互作用弱约1000倍。

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