TAR RNA适体的锁核酸/2'-O-甲基嵌合衍生物的系统筛选。

Systematic screening of LNA/2'-O-methyl chimeric derivatives of a TAR RNA aptamer.

作者信息

Di Primo Carmelo, Rudloff Ivo, Reigadas Sandrine, Arzumanov Andrey A, Gait Michael J, Toulmé Jean-Jacques

机构信息

INSERM U869, Institut Européen de Chimie et Biologie, 2 rue Escarpit, Pessac cedex, F-33607, France.

出版信息

FEBS Lett. 2007 Feb 20;581(4):771-4. doi: 10.1016/j.febslet.2007.01.047. Epub 2007 Jan 30.

DOI:10.1016/j.febslet.2007.01.047

PMID:17276430

Abstract

We synthesized and evaluated by surface plasmon resonance 64 LNA/2'-O-methyl sequences corresponding to all possible combinations of such residues in a kissing aptamer loop complementary to the 6-nt loop of the TAR element of HIV-1. Three combinations of LNA/2'-O-methyl nucleoside analogues where one or two LNA units are located on the 3' side of the aptamer loop display an affinity for TAR below 1nM, i.e. one order of magnitude higher than the parent RNA aptamer. One of these combinations inhibits the TAR-dependent luciferase expression in a cell assay.

摘要

我们通过表面等离子体共振合成并评估了64个与HIV-1的TAR元件6核苷酸环互补的亲吻适配体环中此类残基的所有可能组合相对应的LNA/2'-O-甲基序列。LNA/2'-O-甲基核苷类似物的三种组合（其中一个或两个LNA单元位于适配体环的3'侧）对TAR的亲和力低于1nM，即比亲本RNA适配体高一个数量级。这些组合之一在细胞试验中抑制了TAR依赖性荧光素酶表达。

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TAR RNA适体的锁核酸/2'-O-甲基嵌合衍生物的系统筛选。

Systematic screening of LNA/2'-O-methyl chimeric derivatives of a TAR RNA aptamer.

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