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A magnesium-induced RNA conformational switch at the internal ribosome entry site of hepatitis C virus genome visualized by atomic force microscopy

机译:通过原子力显微镜观察丙型肝炎病毒基因组内部核糖体进入位点的镁诱导的RNA构象转换

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摘要

The 5' untranslated region of hepatitis C virus (HCV) genomic RNA contains an internal ribosome entry site (IRES) element, composed of domains II-IV, which is required for cap-independent translation initiation. Little information on the 3D structure of the whole functional HCV IRES is still available. Here, we use atomic force microscopy to visualize the HCV IRES conformation in its natural sequence context, which includes the upstream domain I and the essential, downstream domains V and VI. The 574 nt-long molecule analyzed underwent an unexpected, Mg2+-induced switch between two alternative conformations: from 'open', elongated morphologies at 0-2 mM Mg2+ concentration to a 'closed', comma-shaped conformation at 4-6 mM Mg2+. This sharp transition, confirmed by gel-shift analysis and partial RNase T1 cleavage, was hindered by the microRNA miR-122. The comma-shaped IRES-574 molecules visualized at 4-6 mM Mg2+ in the absence of miR-122 showed two arms. Our data support that the first arm would contain domain III, while the second one would be composed of domains (I-II)+(V-VI) thanks to a long-range RNA interaction between the I-II spacer and the basal region of domain VI. This reinforces the previously described structural continuity between the HCV IRES and its flanking domains I, V and VI.
机译:丙型肝炎病毒(HCV)基因组RNA的5'非翻译区包含一个内部核糖体进入位点(IRES)元件,该元件由域II-IV组成,这是不依赖帽的翻译起始所必需的。关于整个功能性HCV IRES的3D结构的信息仍然很少。在这里,我们使用原子力显微镜在其自然序列上下文中可视化HCV IRES构象,其中包括上游结构域I和基本的下游结构域V和VI。分析的574 nt长分子经历了Mg2 +诱导的两个替代构象之间的意外转换:从0-2 mM Mg2 +浓度的“开放”,细长形态到4-6 mM Mg2 +的“封闭”,逗号形构型。 。 microRNA miR-122阻止了这种急剧的转变,这种转变是通过凝胶位移分析和部分RNase T1切割证实的。在不存在miR-122的情况下,在4-6 mM Mg2 +处可见的逗号形IRES-574分子显示了两个臂。我们的数据支持第一个臂包含结构域III,而第二个臂则由结构域(I-II)+(V-VI)组成,这要归功于I-II间隔基与基底区域之间的长距离RNA相互作用域VI。这加强了HCV IRES与其侧翼结构域I,V和VI之间的先前描述的结构连续性。

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