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HU Binding to a DNA Four-Way Junction Probed by Főrster Resonance Energy Transfer

机译:胡绑定到DNa四方向交叉探索sun Yatsen通过共振能量转移

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摘要

The Escherichia coli protein, HU, is a non sequence-specific DNA-binding protein that interacts with DNA primarily through electrostatic interactions. In addition to non-specific binding to linear DNA, HU has been shown to bind with nanomolar affinity to discontinuous DNA substrates, such as repair and recombination intermediates. This work specifically examines the HU-four way junction (4WJ) interaction using fluorescence spectroscopic methods. The conformation of the junction in the presence of different counterions was investigated by Förster resonance energy transfer (FRET) measurements, which revealed an ion-type conformational dependence, where Na+ yields the most stacked conformation followed by K+ and Mg2+. HU binding induces a greater degree of stacking in the Na+-stabilized and Mg2+-stabilized junctions but not the K+-stabilized junction, which is attributed to differences in the size of the ionic radii and potential differences in ion binding sites. Interestingly, junction conformation modulates binding affinity, where HU exhibits the lowest affinity for the Mg2+-stabilized form (24 μM−1), which is the least stacked conformation. Protein binding to a mixed population of open and stacked forms of the junction leads to near complete formation of a protein-stabilized stacked-X junction. These results strongly support a model in which HU binds to and stabilizes the stacked-X conformation.

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  • 年(卷),期 -1(50),9
  • 年度 -1
  • 页码 1432–1441
  • 总页数 25
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