Evaluation of different types of end-capping modifications on the stability of oligonucleotides toward 3'- and 5'-exonucleases.

D Pandolfi, F Rauzi, M L Capobianco
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引用次数: 19

Abstract

Synthetic oligonucleotides are increasingly used because of their potential activity as regulators of gene expression. One of their major drawbacks is instability toward nucleases, in particular exonucleases. In this article, we studied some terminal modifications that can enhance exonuclease resistance, such as end-capping with alkylic chains (1,3-propanediol and 1,6-hexanediol), and with a modified nucleotide (2',3'-secouridine). These compounds were compared with the parent (natural) oligodeoxynucleotide and with different analogs containing a progressive number of phosphorothioate linkages. The resistance toward SVPDE and CSPDE (a 3'- and a 5'-exonuclease) was assessed, in vitro, by two independent techniques, UV and HPLC. Our results showed that the stability of all the modified oligonucleotides was at least 12 times that of the parent compound.

不同类型的端盖修饰对寡核苷酸对3′-和5′-外切酶稳定性的影响。
人工合成的寡核苷酸由于其作为基因表达调节因子的潜在活性而被越来越多地使用。它们的主要缺点之一是对核酸酶,特别是外切酶不稳定。在这篇文章中,我们研究了一些末端修饰可以增强抗外切酶能力,例如用烷基链(1,3-丙二醇和1,6-己二醇)和修饰的核苷酸(2',3'-塞库啶)进行末端修饰。这些化合物与母体(天然)寡脱氧核苷酸和不同的类似物进行了比较,这些类似物含有越来越多的磷硫键。通过紫外和高效液相色谱两种独立的技术对SVPDE和CSPDE(3'-和5'-外切酶)的体外抗性进行了评估。结果表明,所有修饰的寡核苷酸的稳定性至少是母体化合物的12倍。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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