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Structural basis for Z-DNA binding and stabilization by the zebrafish Z-DNA dependent protein kinase PKZ

机译:斑马鱼Z-DNA依赖性蛋白激酶PKZ结合和稳定Z-DNA的结构基础

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摘要

The RNA-dependent protein kinase PKR plays a central role in the antiviral defense of vertebrates by shutting down protein translation upon detection of viral dsRNA in the cytoplasm. In some teleost fish, PKZ, a homolog of PKR, performs the same function, but surprisingly, instead of dsRNA binding domains, it harbors two Z-DNA/Z-RNA-binding domains belonging to the Zalpha domain family. Zalpha domains have also been found in other proteins, which have key roles in the regulation of interferon responses such as ADAR1 and DNA-dependent activator of IFN-regulatory factors (DAI) and in viral proteins involved in immune response evasion such as the poxviral E3L and the Cyprinid Herpesvirus 3 ORF112. The underlying mechanism of nucleic acids binding and stabilization by Zalpha domains is still unclear. Here, we present two crystal structures of the zebrafish PKZ Zalpha domain (DrZalpha(PKZ)) in alternatively organized complexes with a (CG)(6) DNA oligonucleotide at 2 and 1.8 A resolution. These structures reveal novel aspects of the Zalpha interaction with DNA, and they give insights on the arrangement of multiple Zalpha domains on DNA helices longer than the minimal binding site.
机译:RNA依赖性蛋白激酶PKR通过在细胞质中检测到病毒dsRNA时关闭蛋白翻译,从而在脊椎动物的抗病毒防御中发挥重要作用。在一些硬骨鱼类中,PKZ是PKR的同系物,具有相同的功能,但令人惊讶的是,它代替了dsRNA结合结构域,而具有两个属于Zalpha域家族的Z-DNA / Z-RNA结合结构域。 Zalpha结构域还存在于其他蛋白质中,这些蛋白质在干扰素应答的调节中起关键作用,例如ADAR1和IFN调节因子(DAI)的DNA依赖性激活剂,以及在涉及免疫应答逃避的病毒蛋白(如痘病毒E3L)中和Cyrpinid疱疹病毒3 ORF112。核酸通过Zalpha域结合和稳定的基本机制仍不清楚。在这里,我们提出了斑马鱼PKZ Zalpha域(DrZalpha(PKZ))的两个晶体结构与(CG)(6)DNA寡核苷酸以2和1.8 A分辨率交替组织的复合体。这些结构揭示了Zalpha与DNA相互作用的新颖方面,并且它们提供了对DNA螺旋上多个Zalpha结构域的排列时间长于最小结合位点的见识。

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