首页> 美国卫生研究院文献>Nucleic Acids Research >Effect of template secondary structure on the inhibition of HIV-1 reverse transcriptase by a pyridinone non-nucleoside inhibitor.
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Effect of template secondary structure on the inhibition of HIV-1 reverse transcriptase by a pyridinone non-nucleoside inhibitor.

机译:模板二级结构对吡啶酮非核苷抑制剂抑制HIV-1逆转录酶的影响。

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摘要

The importance of RNA secondary structure on HIV-1 reverse transcriptase catalyzed polymerization and on the potency of the pyridin-2-one inhibitor 3-(4,7-dichlorobenzoxazol-2-ylmethylamino)-5-ethyl-6-meth ylpyridin-2(1H)-one, L-697,661, were investigated by employing heteromeric primer-template systems. Our data revealed that a stem-loop hairpin secondary structure in the RNA template could lead to strong hindrance of reverse transcription in the reaction catalyzed by HIV-1 reverse transcriptase resulting in the build up of intermediate-length (pause) polymerization products. The presence of L-697,661 greatly enhanced the accumulation of the pause products suggesting that the rate of enzyme translocation from the pause product might be more potently inhibited than polymerization up to the pause site. Model experiments using a synthetic RNA template containing a stem-loop hairpin revealed that the inhibitory potency of L-697, 661 increased 2-fold upon polymerization to within four bases of the secondary structure. Inhibitor potency was enhanced over 6-fold when primer-extension proceeded through the duplex region of the stem-loop.
机译:RNA二级结构对HIV-1逆转录酶催化的聚合反应以及对吡啶-2-酮抑制剂3-(4,7-二氯苯并恶唑-2-基甲基氨基)-5-乙基-6-甲基基吡啶2的效力的重要性(1H)-一,L-697,661,通过使用异源引物-模板系统进行了研究。我们的数据表明,RNA模板中的茎环发夹二级结构可能会导致由HIV-1逆转录酶催化的反应中逆转录的强烈阻碍,从而导致中等长度(暂停)聚合产物的形成。 L-697,661的存在极大地增加了暂停产物的积累,表明从暂停产物中转移酶的速率可能比聚合到暂停位点的抑制作用更强。使用含有茎环发夹的合成RNA模板进行的模型实验显示,聚合后,L-697、661的抑制力增加了2倍,达到二级结构的四个碱基之内。当引物延伸通过茎环的双链体区域时,抑制剂的效力提高了6倍以上。

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