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The crystal structure of the second Z-DNA binding domain of human DAI (ZBP1) in complex with Z-DNA reveals an unusual binding mode to Z-DNA

机译:人DAI的第二个Z-DNA结合结构域(ZBP1)与Z-DNA的晶体结构揭示了与Z-DNA的异常结合方式

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摘要

Mammalian DAI (DNA-dependent activator of IFN-regulatory factors), an activator of the innate immune response, senses cytosolic DNA by using 2 N-terminal Z-DNA binding domains (ZBDs) and a third putative DNA binding domain located next to the second ZBD. Compared with other previously known ZBDs, the second ZBD of human DAI (hZβDAI) shows significant variation in the sequence of the residues that are essential for DNA binding. In this article, the crystal structure of the hZβDAI/Z-DNA complex reveals that hZβDAI has a similar fold to that of other ZBDs, but adopts an unusual binding mode for recognition of Z-DNA. A residue in the first β-strand rather than residues in the β-loop contributes to DNA binding, and part of the (α3) recognition helix adopts a 310 helix conformation. The role of each residue that makes contact with DNA was confirmed by mutational analysis. The 2 ZBDs of DAI can together bind to DNA and both are necessary for full B-to-Z conversion. It is possible that binding 2 DAIs to 1 dsDNA brings about dimerization of DAI that might facilitate DNA-mediated innate immune activation.
机译:哺乳动物DAI(IFN调节因子的DNA依赖性激活剂)是先天性免疫应答的激活剂,它通过使用2个N端Z-DNA结合域(ZBD)和位于细胞旁的第三个推定DNA结合域来感知胞质DNA。第二个ZBD。与其他先前已知的ZBD相比,人DAI的第二个ZBD(hZβDAI)在DNA结合必不可少的残基序列中显示出显着变化。在本文中,hZβDAI/ Z-DNA复合物的晶体结构揭示了hZβDAI与其他ZBD的折叠相似,但采用非常规的结合方式识别Z-DNA。第一个β链中的残基而不是β环中的残基有助于DNA结合,并且(α3)识别螺旋的一部分采用310螺旋构象。通过突变分析证实了与DNA接触的每个残基的作用。 DAI的2个ZBD可以一起与DNA结合,并且都是完全B到Z转换所必需的。将2个DAI与1个dsDNA结合可能导致DAI的二聚化,这可能会促进DNA介导的先天免疫激活。

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