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蛇形菌素的结构研究,一种抗病毒的自由基 S-腺苷甲硫氨酸酶。

Structural studies of viperin, an antiviral radical SAM enzyme.

机构信息

Department of Chemistry and Chemical Biology, Cornell University, Ithaca, NY 14853.

Department of Immunobiology, Yale University School of Medicine, New Haven, CT 06520.

出版信息

Proc Natl Acad Sci U S A. 2017 Jun 27;114(26):6806-6811. doi: 10.1073/pnas.1705402114. Epub 2017 Jun 12.

DOI:10.1073/pnas.1705402114
PMID:28607080
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5495270/
Abstract

Viperin is an IFN-inducible radical -adenosylmethionine (SAM) enzyme that inhibits viral replication. We determined crystal structures of an anaerobically prepared fragment of mouse viperin (residues 45-362) complexed with -adenosylhomocysteine (SAH) or 5'-deoxyadenosine (5'-dAdo) and l-methionine (l-Met). Viperin contains a partial (βα)-barrel fold with a disordered N-terminal extension (residues 45-74) and a partially ordered C-terminal extension (residues 285-362) that bridges the partial barrel to form an overall closed barrel structure. Cys84, Cys88, and Cys91 located after the first β-strand bind a [4Fe-4S] cluster. The active site architecture of viperin with bound SAH (a SAM analog) or 5'-dAdo and l-Met (SAM cleavage products) is consistent with the canonical mechanism of 5'-deoxyadenosyl radical generation. The viperin structure, together with sequence alignments, suggests that vertebrate viperins are highly conserved and that fungi contain a viperin-like ortholog. Many bacteria and archaebacteria also express viperin-like enzymes with conserved active site residues. Structural alignments show that viperin is similar to several other radical SAM enzymes, including the molybdenum cofactor biosynthetic enzyme MoaA and the RNA methyltransferase RlmN, which methylates specific nucleotides in rRNA and tRNA. The viperin putative active site contains several conserved positively charged residues, and a portion of the active site shows structural similarity to the GTP-binding site of MoaA, suggesting that the viperin substrate may be a nucleoside triphosphate of some type.

摘要

Viperin 是一种 IFN 诱导的自由基 - 腺苷甲硫氨酸(SAM)酶,可抑制病毒复制。我们确定了与 - 腺苷同型半胱氨酸(SAH)或 5'-脱氧腺苷(5'-dAdo)和 L-甲硫氨酸(L-Met)结合的鼠源 viperin(残基 45-362)的厌氧制备片段的晶体结构。Viperin 包含一个部分(βα)-桶折叠,带有无序的 N 端延伸(残基 45-74)和部分有序的 C 端延伸(残基 285-362),该延伸将部分桶桥接形成整体封闭桶结构。位于第一个β-链后的 Cys84、Cys88 和 Cys91 结合 [4Fe-4S] 簇。结合 SAH(SAM 类似物)或 5'-dAdo 和 L-Met(SAM 裂解产物)的 Viperin 活性位点结构与 5'-脱氧腺苷自由基生成的典型机制一致。Viperin 结构与序列比对表明,脊椎动物 Viperin 高度保守,真菌含有 Viperin 样同源物。许多细菌和古细菌也表达具有保守活性位点残基的 Viperin 样酶。结构比对表明,Viperin 与其他几种自由基 SAM 酶相似,包括钼辅因子生物合成酶 MoaA 和 RNA 甲基转移酶 RlmN,它们甲基化 rRNA 和 tRNA 中的特定核苷酸。Viperin 假定的活性位点包含几个保守的正电荷残基,活性位点的一部分显示出与 MoaA 的 GTP 结合位点的结构相似性,表明 Viperin 的底物可能是某种类型的核苷三磷酸。

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