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首页> 外文期刊>Nucleic acids research >Footprinting, circular dichroism and UV melting studies on neomycin B binding to the packaging region of human immunodeficiency virus type-1 RNA
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Footprinting, circular dichroism and UV melting studies on neomycin B binding to the packaging region of human immunodeficiency virus type-1 RNA

机译:新霉素B与人免疫缺陷病毒1型RNA包装区域结合的足迹,圆二色性和UV熔融研究

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We have studied the binding of neomycin to a 171mer RNA (ψ-RNA) from the packaging region of the LAI strain of human immunodeficiency virus type-1, HIV-1 (LAI). The RNase I footprinting studies reveal that the primary binding site for the drug is in stem–loop 1, which contains the dimer initiation site of HIV-1. Loading this site with neomycin causes a structural change in the RNA, allowing nucleotides in the neighboring stem–loop 2 to participate in the drug site. Drug binding to secondary sites induces structural changes in other stem–loops of the RNA. Footprinting plots, showing cutting at a site as a function of drug concentration, were analyzed using a two-state model to obtain relative site-specific binding constants. Circular dichroism measurements show that neomycin binding to ψ-RNA changes the intensity of the strong negative CD band at 208 nm, confirming that neomycin induces structural changes. Melting studies of the RNA showed melting transitions in the absence of drug at 28.2, 37.2, 47.4, 55.5 and 60.8°C. Only the first two were affected by drug binding, the reason for this being explained by our analysis.
机译:我们已经研究了新霉素与人免疫缺陷病毒1型HIV-1(LAI)的LAI株包装区域中171mer RNA(ψ-RNA)的结合。 RNase I足迹研究表明,该药物的主要结合位点在茎环1中,其中含有HIV-1的二聚体起始位点。在该位点上加载新霉素会引起RNA的结构变化,从而使邻近的茎环2中的核苷酸参与药物位点。药物与次级位点的结合会诱导RNA其他茎环的结构变化。使用二态模型分析了足迹图,该图显示了一个部位的切割与药物浓度的关系,从而获得了相对于部位的特定结合常数。圆二色性测量表明,新霉素与ψ-RNA的结合改变了208 nm处强负CD带的强度,证实了新霉素诱导了结构变化。 RNA的融解研究显示,在无药物的情况下,在28.2、37.2、47.4、55.5和60.8°C时融解转变。只有前两个受到药物结合的影响,我们的分析解释了其原因。

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