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首页> 外文期刊>Nucleic Acids Research >The structures of non-CG-repeat Z-DNAs co-crystallized with the Z-DNA-binding domain, hZ alpha(ADAR1)
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The structures of non-CG-repeat Z-DNAs co-crystallized with the Z-DNA-binding domain, hZ alpha(ADAR1)

机译:非CG重复Z-DNA的结构与Z-DNA结合域hZ alpha(ADAR1)共结晶

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摘要

The Z-DNA conformation preferentially occurs at alternating purine-pyrimidine repeats, and is specifically recognized by Z alpha domains identified in several Z-DNA-binding proteins. The binding of Z alpha to foreign or chromosomal DNA in various sequence contexts is known to influence various biological functions, including the DNA-mediated innate immune response and transcriptional modulation of gene expression. For these reasons, understanding its binding mode and the conformational diversity of Z alpha bound Z-DNAs is of considerable importance. However, structural studies of Z alpha bound Z-DNA have been mostly limited to standard CG-repeat DNAs. Here, we have solved the crystal structures of three representative non-CG repeat DNAs, d(CACGTG)(2), d(CGTACG)(2) and d(CGGCCG)(2) complexed to hZ alpha(ADAR1) and compared those structures with that of hZ alpha(ADAR1)/d(CGCGCG)(2) and the Z alpha-free Z-DNAs. hZ alpha(ADAR1) bound to each of the three Z-DNAs showed a well conserved binding mode with very limited structural deviation irrespective of the DNA sequence, although varying numbers of residues were in contact with Z-DNA. Z-DNAs display less structural alterations in the Z alpha-bound state than in their free form, thereby suggesting that conformational diversities of Z-DNAs are restrained by the binding pocket of Z alpha. These data suggest that Z-DNAs are recognized by Z alpha through common conformational features regardless of the sequence and structural alterations.
机译:Z-DNA构象优先出现在交替的嘌呤-嘧啶重复序列上,并被几种Z-DNA结合蛋白中鉴定出的Z alpha结构域特异性识别。已知在各种序列背景下Zα与外来或染色体DNA的结合会影响各种生物学功能,包括DNA介导的先天免疫应答和基因表达的转录调节。由于这些原因,了解其结合模式和与Zα结合的Z-DNA的构象多样性非常重要。但是,与Z alpha结合的Z-DNA的结构研究主要限于标准CG重复DNA。在这里,我们解决了与hZ alpha(ADAR1)络合的三个代表性非CG重复DNA d(CACGTG)(2),d(CGTACG)(2)和d(CGGCCG)(2)的晶体结构,并进行了比较具有hZ alpha(ADAR1)/ d(CGCGCG)(2)和不含Z alpha的Z-DNA的结构。结合到三个Z-DNA的hZ alpha(ADAR1)表现出良好的保守结合模式,无论DNA序列如何,结构偏差都非常有限,尽管与Z-DNA接触的残基数量不同。 Z-DNA在Zα-结合状态下的结构变化少于其自由形式,从而表明Z-DNA的构象多样性受Zα的结合口袋限制。这些数据表明,Z-DNA可通过共同的构象特征被Z alpha识别,而与序列和结构改变无关。

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