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ST1710–DNA complex crystal structure reveals the DNA binding mechanism of the MarR family of regulators

机译:ST1710–DNA复杂的晶体结构揭示了MarR调控因子家族的DNA结合机制

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摘要

ST1710, a member of the multiple antibiotic resistance regulator (MarR) family of regulatory proteins in bacteria and archaea, plays important roles in development of antibiotic resistance, a global health problem. Here, we present the crystal structure of ST1710 from Sulfolobus tokodaii strain 7 complexed with salicylate, a well-known inhibitor of MarR proteins and the ST1710 complex with its promoter DNA, refined to 1.8 and 2.10 Å resolutions, respectively. The ST1710–DNA complex shares the topology of apo-ST1710 and MarR proteins, with each subunit containing a winged helix-turn-helix (wHtH) DNA binding motif. Significantly large conformational changes occurred upon DNA binding and in each of the dimeric monomers in the asymmetric unit of the ST1710–DNA complex. Conserved wHtH loop residues interacting with the bound DNA and mutagenic analysis indicated that R89, R90 and K91 were important for DNA recognition. Significantly, the bound DNA exhibited a new binding mechanism.
机译:ST1710是细菌和古细菌中多种抗生素抗性调节剂(MarR)调节蛋白家族的成员,在全球耐药性问题抗生素抗性的发展中起着重要作用。在这里,我们介绍了来自Sulfolobus tokodaii菌株7的ST1710的晶体结构,该菌株与水杨酸盐(一种著名的MarR蛋白抑制剂)复合,以及具有启动子DNA的ST1710复合物,分别精制到1.8和2.10Å的分辨率。 ST1710–DNA复合体具有apo-ST1710和MarR蛋白的拓扑结构,每个亚基均含有带翼的螺旋-螺旋-螺旋(wHtH)DNA结合基序。 DNA结合后以及ST1710–DNA复合体不对称单元中的每个二聚体单体中均发生了显着的构象变化。保守的wHtH环残基与结合的DNA相互作用,诱变分析表明R89,R90和K91对于DNA识别很重要。显着地,结合的DNA表现出新的结合机制。

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