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RNA 3'-磷酸环化酶(RtcA)催化 DNA 和 RNA 5'-单磷酸末端的连接酶样腺苷酰化反应。

RNA 3'-phosphate cyclase (RtcA) catalyzes ligase-like adenylylation of DNA and RNA 5'-monophosphate ends.

机构信息

Molecular Biology Program, Sloan-Kettering Institute, New York, New York 10065, USA.

出版信息

J Biol Chem. 2011 Feb 11;286(6):4117-22. doi: 10.1074/jbc.M110.196766. Epub 2010 Nov 22.

Abstract

RNA 3'-phosphate cyclase (Rtc) enzymes are a widely distributed family that catalyze the synthesis of RNA 2',3'-cyclic phosphate ends via an ATP-dependent pathway comprising three nucleotidyl transfer steps: reaction of Rtc with ATP to form a covalent Rtc-(histidinyl-N)-AMP intermediate and release PP(i); transfer of AMP from Rtc to an RNA 3'-phosphate to form an RNA(3')pp(5')A intermediate; and attack by the terminal nucleoside O2' on the 3'-phosphate to form an RNA 2',3'-cyclic phosphate product and release AMP. The chemical transformations of the cyclase pathway resemble those of RNA and DNA ligases, with the key distinction being that ligases covalently adenylylate 5'-phosphate ends en route to phosphodiester synthesis. Here we show that the catalytic repertoire of RNA cyclase overlaps that of ligases. We report that Escherichia coli RtcA catalyzes adenylylation of 5'-phosphate ends of DNA or RNA strands to form AppDNA and AppRNA products. The polynucleotide 5' modification reaction requires the His(309) nucleophile, signifying that it proceeds through a covalent RtcA-AMP intermediate. We established this point directly by demonstrating transfer of [(32)P]AMP from RtcA to a pDNA strand. RtcA readily adenylylated the 5'-phosphate at a 5'-PO(4)/3'-OH nick in duplex DNA but was unable to covert the nicked DNA-adenylate to a sealed phosphodiester. Our findings raise the prospect that cyclization of RNA 3'-ends might not be the only biochemical pathway in which Rtc enzymes participate; we discuss scenarios in which the 5'-adenylyltransferase of RtcA might play a role.

摘要

RNA 3'-磷酸环化酶(Rtc)酶是一个广泛分布的家族,通过一个依赖于 ATP 的途径催化 RNA 2',3'-环磷酸末端的合成,该途径包括三个核苷酸转移步骤:Rtc 与 ATP 反应形成共价 Rtc-(组氨酰基-N)-AMP 中间产物并释放 PP(i);AMP 从 Rtc 转移到 RNA 3'-磷酸上形成 RNA(3')pp(5')A 中间产物;最后末端核苷 O2'攻击 3'-磷酸形成 RNA 2',3'-环磷酸产物并释放 AMP。环化酶途径的化学转化类似于 RNA 和 DNA 连接酶的转化,关键区别在于连接酶在磷酸二酯合成过程中共价腺苷酸化 5'-磷酸末端。在这里,我们表明 RNA 环化酶的催化谱与连接酶重叠。我们报告说,大肠杆菌 RtcA 催化 DNA 或 RNA 链的 5'-磷酸末端的腺苷酸化,形成 AppDNA 和 AppRNA 产物。多核苷酸 5'修饰反应需要 His(309)亲核试剂,这表明它通过共价 RtcA-AMP 中间产物进行。我们通过直接证明 [(32)P]AMP 从 RtcA 转移到 pDNA 链来证明这一点。RtcA 容易腺苷酸化双链 DNA 中的 5'-磷酸末端的 5'-PO(4)/3'-OH 缺口,但无法将缺口 DNA-腺苷酸转化为封闭的磷酸二酯。我们的发现提出了这样一种可能性,即 RNA 3'-末端的环化可能不是 Rtc 酶参与的唯一生化途径;我们讨论了 RtcA 的 5'-腺苷酰转移酶可能发挥作用的情况。

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