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EMBO J. 1997 May 15;16(10):2955-67. doi: 10.1093/emboj/16.10.2955.
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Crystal structure of RNA 3'-terminal phosphate cyclase, a ubiquitous enzyme with unusual topology.RNA 3'-末端磷酸环化酶的晶体结构,一种拓扑结构独特的普遍存在的酶。
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本文引用的文献

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Cell-free circularization of viroid progeny RNA by an RNA ligase from wheat germ.小麦胚 RNA 连接酶对类病毒前体 RNA 的无细胞环化作用。
Science. 1982 Sep 17;217(4565):1147-9. doi: 10.1126/science.217.4565.1147.
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Complete genome sequence of the methanogenic archaeon, Methanococcus jannaschii.产甲烷古菌詹氏甲烷球菌的全基因组序列
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SR proteins and splicing control.SR蛋白与剪接调控。
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RNA capping enzyme and DNA ligase: a superfamily of covalent nucleotidyl transferases.RNA 封端酶与 DNA 连接酶:共价核苷酸转移酶超家族
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Sequence-specific cleavage of DNA via nucleophilic attack of hydrogen peroxide, assisted by Flp recombinase.在Flp重组酶的辅助下,通过过氧化氢的亲核攻击实现DNA的序列特异性切割。
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Mammalian U6 small nuclear RNA undergoes 3' end modifications within the spliceosome.哺乳动物U6小核RNA在剪接体内进行3'端修饰。
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Pre-tRNA splicing: variation on a theme or exception to the rule?前体tRNA剪接:主题的变体还是规则的例外?
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8
The covalent eukaryotic topoisomerase I-DNA intermediate catalyzes pH-dependent hydrolysis and alcoholysis.共价真核拓扑异构酶I-DNA中间体催化pH依赖性水解和醇解。
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9
Purification of CpG islands using a methylated DNA binding column.使用甲基化DNA结合柱纯化CpG岛。
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10
CLUSTAL W: improving the sensitivity of progressive multiple sequence alignment through sequence weighting, position-specific gap penalties and weight matrix choice.CLUSTAL W:通过序列加权、位置特异性空位罚分和权重矩阵选择提高渐进多序列比对的灵敏度。
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人类RNA 3'-末端磷酸环化酶是真核生物、细菌和古细菌中保守的一个新蛋白质家族的成员。

The human RNA 3'-terminal phosphate cyclase is a member of a new family of proteins conserved in Eucarya, Bacteria and Archaea.

作者信息

Genschik P, Billy E, Swianiewicz M, Filipowicz W

机构信息

Friedrich Miescher-Institut, Basel, Switzerland.

出版信息

EMBO J. 1997 May 15;16(10):2955-67. doi: 10.1093/emboj/16.10.2955.

DOI:10.1093/emboj/16.10.2955
PMID:9184239
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1169903/
Abstract

RNA 3'-terminal phosphate cyclase catalyses the ATP-dependent conversion of the 3'-phosphate to a 2',3'-cyclic phosphodiester at the end of RNA. The physiological function of the cyclase is not known, but the enzyme could be involved in the maintenance of cyclic ends in tRNA splicing intermediates or in the cyclization of the 3' end of U6 snRNA. In this work, we describe cloning of the human cyclase cDNA. The purified bacterially overexpressed protein underwent adenylylation in the presence of [alpha-32P]ATP and catalysed cyclization of the 3'-terminal phosphate in different RNA substrates, consistent with previous findings. Comparison of oligoribonucleotides and oligodeoxyribonucleotides of identical sequence demonstrated that the latter are approximately 500-fold poorer substrates for the enzyme. In Northern analysis, the cyclase was expressed in all analysed mammalian tissues and cell lines. Indirect immunofluorescence, performed with different transfected mammalian cell lines, showed that this protein is nuclear, with a diffuse nucleoplasmic localization. The sequence of the human cyclase has no apparent motifs in common with any proteins of known function. However, inspection of the databases identified proteins showing strong similarity to the enzyme, originating from as evolutionarily distant organisms as yeast, plants, the bacterium Escherichia coli and the archaeon Methanococcus jannaschii. The overexpressed E. coli protein has cyclase activity similar to that of the human enzyme. The conservation of the RNA 3'-terminal phosphate cyclase among Eucarya, Bacteria and Archaea argues that the enzyme performs an important function in RNA metabolism.

摘要

RNA 3'-末端磷酸环化酶催化RNA末端3'-磷酸依赖ATP转化为2',3'-环磷酸二酯。该环化酶的生理功能尚不清楚,但该酶可能参与tRNA剪接中间体中环化末端的维持或U6 snRNA 3'末端的环化。在这项工作中,我们描述了人类环化酶cDNA的克隆。纯化的细菌过表达蛋白在[α-32P]ATP存在下进行腺苷酸化,并催化不同RNA底物中3'-末端磷酸的环化,这与先前的发现一致。相同序列的寡核糖核苷酸和寡脱氧核糖核苷酸的比较表明,后者作为该酶的底物时活性约低500倍。在Northern分析中,环化酶在所有分析的哺乳动物组织和细胞系中均有表达。对不同转染的哺乳动物细胞系进行间接免疫荧光分析表明,该蛋白定位于细胞核,呈弥漫性核质定位。人类环化酶的序列与任何已知功能的蛋白质均无明显的共有基序。然而,对数据库的检索发现了与该酶具有高度相似性的蛋白质,这些蛋白质来源于进化距离较远的生物,如酵母、植物、大肠杆菌和詹氏甲烷球菌。过表达的大肠杆菌蛋白具有与人类酶相似的环化酶活性。真核生物、细菌和古细菌中RNA 3'-末端磷酸环化酶的保守性表明该酶在RNA代谢中发挥着重要作用。