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斑马鱼 Z-DNA 依赖蛋白激酶 PKZ 结合和稳定 Z-DNA 的结构基础。

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

机构信息

Instituto Gulbenkian de Ciência, Rua Quinta Grande 6, 2780-156 Oeiras, Portugal.

出版信息

Nucleic Acids Res. 2013 Nov;41(21):9924-33. doi: 10.1093/nar/gkt743. Epub 2013 Aug 23.

Abstract

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 Å 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.

摘要

依赖 RNA 的蛋白激酶 PKR 在脊椎动物的抗病毒防御中发挥核心作用,当细胞质中检测到病毒 dsRNA 时,它会关闭蛋白质翻译。在一些硬骨鱼中,PKZ 是 PKR 的同源物,具有相同的功能,但令人惊讶的是,它没有 dsRNA 结合结构域,而是拥有两个属于 Zalpha 结构域家族的 Z-DNA/Z-RNA 结合结构域。Zalpha 结构域也存在于其他具有干扰素反应调节关键作用的蛋白质中,如 ADAR1 和 DNA 依赖性干扰素调节因子激活物(DAI),以及参与免疫反应逃避的病毒蛋白,如痘病毒 E3L 和鲤鱼疱疹病毒 3 ORF112。Zalpha 结构域结合和稳定核酸的潜在机制尚不清楚。在这里,我们展示了两种斑马鱼 PKZ Zalpha 结构域(DrZalpha(PKZ))的晶体结构,它们以不同的方式与(CG)6 DNA 寡核苷酸形成复合物,分辨率分别为 2 和 1.8 Å。这些结构揭示了 Zalpha 与 DNA 相互作用的新方面,并提供了关于多个 Zalpha 结构域在长于最小结合位点的 DNA 螺旋上的排列的见解。

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