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首页> 外文期刊>Journal of Molecular Biology >H-NS Oligomerization Domain Structure Reveals the Mechanism for High Order Self-association of the Intact Protein.
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H-NS Oligomerization Domain Structure Reveals the Mechanism for High Order Self-association of the Intact Protein.

机译:H-NS寡聚域结构揭示了完整蛋白的高阶自缔合的机制。

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摘要

H-NS plays a role in condensing DNA in the bacterial nucleoid. This 136 amino acid protein comprises two functional domains separated by a flexible linker. High order structures formed by the N-terminal oligomerization domain (residues 1-89) constitute the basis of a protein scaffold that binds DNA via the C-terminal domain. Deletion of residues 57-89 or 64-89 of the oligomerization domain precludes high order structure formation, yielding a discrete dimer. This dimerization event represents the initial event in the formation of high order structure. The dimers thus constitute the basic building block of the protein scaffold. The three-dimensional solution structure of one of these units (residues 1-57) has been determined. Activity of these structural units is demonstrated by a dominant negative effect on high order structure formation on addition to the full length protein. Truncated and site-directed mutant forms of the N-terminal domain of H-NS reveal how the dimeric unit self-associates in a head-to-tail manner and demonstrate the importance of secondary structure in this interaction to form high order structures. A model is presented for the structural basis for DNA packaging in bacterial cells.
机译:H-NS在冷凝细菌核苷中的DNA中发挥作用。该136个氨基酸的蛋白质包含被柔性接头隔开的两个功能域。由N末端寡聚结构域(残基1-89)形成的高阶结构构成了通过C末端结构域结合DNA的蛋白质支架的基础。寡聚化结构域的残基57-89或64-89的删除排除了高阶结构的形成,从而产生了离散的二聚体。该二聚化事件代表了高阶结构形成中的初始事件。因此,二聚体构成蛋白质支架的基本构件。已确定这些单元之一(残基1-57)的三维溶液结构。这些结构单元的活性通过在添加全长蛋白质时对高阶结构形成的显性负作用来证明。 H-NS的N末端结构域的截断和定点突变形式揭示了二聚体单元如何以头到尾的方式自缔合,并证明了二级结构在这种相互作用中形成高阶结构的重要性。提出了用于细菌细胞中DNA包装的结构基础的模型。

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