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小球藻病毒DNA连接酶连接链的特异性和保真度

Specificity and fidelity of strand joining by Chlorella virus DNA ligase.

作者信息

Sriskanda V, Shuman S

机构信息

Molecular Biology Program, Sloan-Kettering Institute, New York, NY 10021, USA.

出版信息

Nucleic Acids Res. 1998 Aug 1;26(15):3536-41. doi: 10.1093/nar/26.15.3536.

Abstract

Chlorella virus PBCV-1 DNA ligase seals nicked duplex DNA substrates consisting of a 5'-phosphate-terminated strand and a 3'-hydroxyl-terminated strand annealed to a bridging template strand, but cannot ligate a nicked duplex composed of two DNAs annealed on an RNA template. Whereas PBCV-1 ligase efficiently joins a 3'-OH RNA to a 5'-phosphate DNA, it is unable to join a 3'-OH DNA to a 5'-phosphate RNA. The ligase discriminates at the substrate binding step between nicked duplexes containing 5'-phosphate DNA versus 5'-phosphate RNA strands. PBCV-1 ligase readily seals a nicked duplex DNA containing a single ribonucleotide substitution at the reactive 5'-phosphate end. These results suggest a requirement for a B-form helical conformation of the polynucleotide on the 5'-phosphate side of the nick. Single base mismatches at the nick exert disparate effects on DNA ligation efficiency. PBCV-1 ligase tolerates mismatches involving the 5'-phosphate nucleotide, with the exception of 5'-A:G and 5'-G:A mispairs, which reduce ligase activity by two orders of magnitude. Inhibitory configurations at the 3'-OH nucleotide include 3'-G:A, 3'-G:T, 3'-T:T, 3'-A:G, 3'-G:G, 3'-A:C and 3'-C:C. Our findings indicate that Chlorella virus DNA ligase has the potential to affect genome integrity by embedding ribonucleotides in viral DNA and by sealing nicked molecules with mispaired ends, thereby generating missense mutations.

摘要

小球藻病毒PBCV-1 DNA连接酶可封闭带切口的双链DNA底物,该底物由一条5'-磷酸末端链和一条与桥接模板链退火的3'-羟基末端链组成,但无法连接由两条在RNA模板上退火的DNA组成的带切口双链体。虽然PBCV-1连接酶能有效地将3'-OH RNA与5'-磷酸DNA连接起来,但它无法将3'-OH DNA与5'-磷酸RNA连接。该连接酶在底物结合步骤中区分含有5'-磷酸DNA链与5'-磷酸RNA链的带切口双链体。PBCV-1连接酶很容易封闭在反应性5'-磷酸末端含有单个核糖核苷酸取代的带切口双链DNA。这些结果表明,在切口的5'-磷酸一侧,多核苷酸需要呈B型螺旋构象。切口处的单碱基错配对DNA连接效率有不同影响。PBCV-1连接酶可容忍涉及5'-磷酸核苷酸的错配,但5'-A:G和5'-G:A错配除外,这两种错配会使连接酶活性降低两个数量级。3'-OH核苷酸处的抑制性构型包括3'-G:A、3'-G:T、3'-T:T、3'-A:G、3'-G:G、3'-A:C和3'-C:C。我们的研究结果表明,小球藻病毒DNA连接酶有可能通过将核糖核苷酸嵌入病毒DNA以及封闭末端错配的带切口分子来影响基因组完整性,从而产生错义突变。

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