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3'-Me-α-L-LNA 的合成及生物物理评估 - α-L-LNA 双链中小沟中的取代。

Synthesis and biophysical evaluation of 3'-Me-α-L-LNA - Substitution in the minor groove of α-L-LNA duplexes.

机构信息

Department of Medicinal Chemistry, Isis Pharmaceuticals, 1891 Rutherford Road, Carlsbad, CA 92008, United States.

出版信息

Bioorg Med Chem Lett. 2011 Aug 15;21(16):4690-4. doi: 10.1016/j.bmcl.2011.06.104. Epub 2011 Jun 30.

Abstract

The synthesis and biophysical evaluation of 3'-Me-α-L-LNA is reported. The synthesis of the nucleoside building block phosphoramidite was accomplished starting from diacetone glucose. The 3'-Me group was introduced in the desired configuration by hydride mediated opening of an exocyclic epoxide. Inversion of the 2'-hydroxyl group was achieved by means of an oxidation/reduction sequence followed by cyclization onto a 5'-leaving group to assemble the [2.2.1] ring system. Biophysical evaluation of 3'-Me-α-L-LNA modified oligonucleotides showed good duplex thermal stabilizing properties which were similar to α-L-LNA. Mismatch discrimination experiments revealed that 3'-Me-α-L-LNA possess slightly enhanced discrimination properties for the GU wobble base-pair as compared to related nucleic acid analogs.

摘要

报道了 3'-Me-α-L-LNA 的合成和生物物理评价。核苷碱基磷酸酯的合成是从二丙酮葡萄糖开始的。通过氢化物介导的环外环氧化物开环,以所需的构型引入 3'-Me 基团。通过氧化/还原序列将 2'-羟基反转,然后环化到 5'-离去基团上,以组装 [2.2.1] 环系统。3'-Me-α-L-LNA 修饰的寡核苷酸的生物物理评价表明,其双链体热稳定性与α-L-LNA 相似。错配识别实验表明,与相关的核酸类似物相比,3'-Me-α-L-LNA 对 GU 摆动碱基对具有略微增强的识别特性。

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