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SYNTHESIS OF 2'-MODIFIED NUCLEOTIDES AND THEIR INCORPORATION INTO HAMMERHEAD RIBOZYMES

机译:2'修饰的核苷酸的合成及其与锤头状核酶的结合

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Several 2'-modified ribonucleoside phosphoramidites have been prepared for structure-activity studies of the hammerhead ribozyme, The aim of these studies was to design and synthesize catalytically active and nuclease-resistant ribozymes, Synthetic schemes for stereoselective synthesis of the R isomer of 2'-deoxy-2'-C-allyl uridine and cytidine phosphoramidites, based on the Keck allylation procedure, were developed, Protection of the 2'-amino group in 2'-deoxy-2'-aminouridine was optimized and a method for the convenient preparation of 5'-O-dimethoxytrityl-2'-deoxy-2'-phthalimidouridine 3'-O-(2-cyanoethyl-N,N-diisopropylphosphoramidite) was developed, During the attempted preparation of the 2'-O-t-butyldimethylsilyl-3'-O-phosphoramidite of arabinouridine a reversed regioselectivity in the silylation reaction, compared with the published procedure, was observed, as well as the unexpected formation of the 2,2'-anhydronucleoside. A possible mechanism for this cyclization is proposed, The synthesis of 2'-deoxy-2'-methylene and 2'-deoxy-2'-difluoromethylene uridine phosphoramidites is described, Based on a '5-ribose' model for essential 2'-hydroxyls in the hammerhead ribozyme these 2'-modified monomers were incorporated at positions U4 and/or U7 of the catalytic core, A number of these ribozymes had almost wild-type catalytic activity and improved stability in human serum, compared with an all-RNA molecule.
机译:已经制备了几种2'-修饰的核糖核苷亚磷酰胺用于锤头状核酶的结构活性研究,这些研究的目的是设计和合成催化活性和耐核酸酶的核酶,用于2'R异构体立体选择性合成的合成方案。基于Keck烯丙基化方法,开发了-deoxy-2'-C-烯丙基尿苷和胞苷亚磷酰胺,优化了2'-deoxy-2'-氨基尿苷中2'-氨基的保护作用,并提出了一种方便的方法开发了5'-O-二甲氧基三苯甲基-2'-脱氧-2'-邻苯二甲酰亚胺基吡啶的制备方法,开发了2'-Ot-丁基二甲基甲硅烷基-与公开的方法相比,观察到了阿拉伯脲的3'-O-亚磷酰胺在甲硅烷基化反应中的区域选择性反转,以及意外地形成了2,2'-脱水核苷。提出了这种环化的可能机理,基于基本2'-的'5-核糖'模型,描述了2'-脱氧-2'-亚甲基和2'-脱氧-2'-二氟亚甲基尿苷亚磷酰胺的合成。在锤头状核酶中,这些2'修饰的单体中的羟基被并入催化核心的U4和/或U7位置。与全RNA相比,这些核酶中的许多具有几乎野生型的催化活性并在人血清中具有更高的稳定性。分子。

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