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真核生物 Box C/D 甲基化机制具有两个非对称的蛋白质组装位点。

Eukaryotic Box C/D methylation machinery has two non-symmetric protein assembly sites.

机构信息

Institute for Organic Chemistry and Centre of Biomolecular Drug Research (BMWZ), Leibniz University Hannover, 30167, Hannover, Lower Saxony, Germany.

Department of Structure and Function of Proteins, Helmholtz Centre of Infection Research, 38124, Braunschweig, Lower Saxony, Germany.

出版信息

Sci Rep. 2021 Sep 2;11(1):17561. doi: 10.1038/s41598-021-97030-y.

Abstract

Box C/D ribonucleoprotein complexes are RNA-guided methyltransferases that methylate the ribose 2'-OH of RNA. The central 'guide RNA' has box C and D motifs at its ends, which are crucial for activity. Archaeal guide RNAs have a second box C'/D' motif pair that is also essential for function. This second motif is poorly conserved in eukaryotes and its function is uncertain. Conflicting literature data report that eukaryotic box C'/D' motifs do or do not bind proteins specialized to recognize box C/D-motifs and are or are not important for function. Despite this uncertainty, the architecture of eukaryotic 2'-O-methylation enzymes is thought to be similar to that of their archaeal counterpart. Here, we use biochemistry, X-ray crystallography and mutant analysis to demonstrate the absence of functional box C'/D' motifs in more than 80% of yeast guide RNAs. We conclude that eukaryotic Box C/D RNPs have two non-symmetric protein assembly sites and that their three-dimensional architecture differs from that of archaeal 2'-O-methylation enzymes.

摘要

Box C/D 核糖核蛋白复合物是 RNA 指导的甲基转移酶,可使 RNA 的核糖 2'-OH 甲基化。中央“指导 RNA”的两端具有 Box C 和 D 基序,这对于其活性至关重要。古菌的指导 RNA 具有第二个 Box C'/D' 基序对,对于功能也是必不可少的。该第二个基序在真核生物中保守性很差,其功能不确定。相互矛盾的文献数据报告表明,真核生物的 Box C'/D' 基序确实或确实不与专门识别 Box C/D 基序的蛋白质结合,并且对于功能确实或确实不重要。尽管存在这种不确定性,但人们认为真核生物 2'-O-甲基化酶的结构与它们的古菌对应物相似。在这里,我们使用生物化学、X 射线晶体学和突变分析来证明超过 80%的酵母指导 RNA 中不存在功能性 Box C'/D' 基序。我们得出的结论是,真核生物 Box C/D RNPs 具有两个不对称的蛋白质组装位点,其三维结构与古菌 2'-O-甲基化酶不同。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/dcf5/8413462/41fa3df63412/41598_2021_97030_Fig1_HTML.jpg

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