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Structure and Cooperativity of the Cytosolic Domain of the CorA Mg2+ Channel from Escherichia coli

机译:来自大肠杆菌的Cora Mg2 +通道的细胞溶质结构域的结构和合作

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摘要

Structures of the Mg2+ bound (closed) and apo (open) states of CorA suggests that channel gating is accomplished by rigid-body motions between symmetric and asymmetric assemblies of the cytosolic portions of the five subunits in response to ligand (Mg2+) binding/unbinding at interfacial sites. Here, we structurally and biochemically characterize the isolated cytosolic domain from Escherichia coli CorA. The data reveal an Mg2+-ligand binding site located in a novel position between each of the five subunits and two Mg2+ ions trapped inside the pore. Soaking experiments show that cobalt hexammine outcompetes Mg2+ at the pore site closest to the membrane. This represents the first structural information of how an analog of hexa-hydrated Mg2+ (and competitive inhibitor of CorA) associates to the CorA pore. Biochemical data on the isolated cytoplasmic domain and full-length protein suggests that gating of the CorA channel is governed cooperatively.
机译:Cora的Mg2 +结合(闭合)和apo(开放)态的结构表明,通道门控通过响应于配体(Mg2 +)结合/解除粘连的五个亚基的胞质部分的对称和不对称组件之间的刚性和不对称组件之间的刚体运动而完成 在界面位点。 在这里,我们在大肠杆菌Coli Cora结构和生物化学地表征分离的细胞溶胶结构域。 该数据揭示了位于五个亚基之间的每一个与孔内的两个Mg2 +离子之间的新位置之间的Mg2 + -ligand结合位点。 浸泡实验表明,钴Hexammine在最接近膜的孔隙位点处脱位Mg2 +。 这代表了如何为Cora孔的六曲水合Mg2 +(和Cora竞争性抑制剂)的类似结构信息。 分离的细胞质结构域和全长蛋白质的生化数据表明,Cora通道的门控是合作的治理。

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  • 来源
    《Structure》 |2017年第8期|共16页
  • 作者单位

    Stockholm Univ Ctr Biomembrane Res Dept Biochem &

    Biophys S-10691 Stockholm Sweden;

    Stockholm Univ Ctr Biomembrane Res Dept Biochem &

    Biophys S-10691 Stockholm Sweden;

    Stockholm Univ Ctr Biomembrane Res Dept Biochem &

    Biophys S-10691 Stockholm Sweden;

    Stockholm Univ Ctr Biomembrane Res Dept Biochem &

    Biophys S-10691 Stockholm Sweden;

    Stockholm Univ Ctr Biomembrane Res Dept Biochem &

    Biophys S-10691 Stockholm Sweden;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 分子生物学;
  • 关键词

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