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DNA靶标上的三链体形成:如何选择寡核苷酸。

Triplex formation on DNA targets: how to choose the oligonucleotide.

作者信息

Vekhoff Pierre, Ceccaldi Alexandre, Polverari David, Pylouster Jean, Pisano Claudio, Arimondo Paola B

机构信息

UMR 5153 CNRS, Museum National d'Histoire Naturelle USM0503, 43 rue Cuvier, 75231 Paris cedex 05, France.

出版信息

Biochemistry. 2008 Nov 25;47(47):12277-89. doi: 10.1021/bi801087g.

Abstract

Triplex-forming oligonucleotides (TFOs) are sequence-specific DNA binders. TFOs provide a tool for controlling gene expression or, when attached to an appropriate chemical reagent, for directing DNA damage. Here, we report a set of rules for predicting the best out of five different triple-helical binding motifs (TM, UM, GA, GT, and GU, where M is 5-methyldeoxycytidine and U is deoxyuridine) by taking into consideration the sequence composition of the underlying duplex target. We tested 11 different triplex targets present in genes having an oncogenic role. The rules have predictive power and are very useful in the design of TFOs for antigene applications. Briefly, we retained motifs GU and TM, and when they do form a triplex, TFOs containing G and U are preferred over those containing T and M. In the case of the G-rich TFOs, triplex formation is principally dependent on the percentage of G and the length of the TFO. In the case of the pyrimidine motif, replacement of T with U is destabilizing; triplex formation is dependent on the percentage of T and destabilized by the presence of several contiguous M residues. An equation to choose between a GU and TM motif is given.

摘要

三链形成寡核苷酸(TFOs)是序列特异性DNA结合剂。TFOs为控制基因表达提供了一种工具,或者当与适当的化学试剂连接时,用于引导DNA损伤。在这里,我们报告了一套规则,通过考虑潜在双链靶标的序列组成,从五个不同的三链螺旋结合基序(TM、UM、GA、GT和GU,其中M是5-甲基脱氧胞苷,U是脱氧尿苷)中预测最佳基序。我们测试了存在于具有致癌作用的基因中的11个不同的三链靶标。这些规则具有预测能力,在设计用于反基因应用的TFOs时非常有用。简而言之,我们保留了GU和TM基序,当它们确实形成三链体时,含有G和U的TFOs比含有T和M的TFOs更受青睐。对于富含G的TFOs,三链体形成主要取决于G的百分比和TFO的长度。对于嘧啶基序,用U取代T会使结构不稳定;三链体形成取决于T的百分比,并因几个连续M残基的存在而不稳定。给出了在GU和TM基序之间进行选择的方程式。

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