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Characterisation of antibody-binding RNAs selected from structurally constrained libraries.

机译:表征选自结构受限文库的抗体结合RNA。

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摘要

Constrained RNA libraries of limited sequence complexity were constructed and used to select RNA molecules binding to the antigen binding site of an anti-ferritin antibody. The sequences required as primer-binding sites for the selection cycle were designed to form a predictable secondary structure, which greatly facilitated the characterisation of the secondary structures of the selected RNAs. RNA-antibody interactions were studied by real-time interaction analysis to study the dynamic aspects of binding and by circular dichroism spectroscopy to search for conformational changes upon binding. The selected RNAs were analysed with a binding site sequestering assay and were shown to compete with ferritin for binding to the antigen-binding site. The experiments described here indicate that the introduction of strong structural constraints does not have to interfere with the ability to select tightly and specifically binding RNA-molecules.
机译:构建具有有限序列复杂性的受约束的RNA文库,并将其用于选择与抗铁蛋白抗体的抗原结合位点结合的RNA分子。选择循环所需的引物结合位点所需的序列,以形成可预测的二级结构,从而大大促进了所选RNA二级结构的表征。通过实时相互作用分析来研究RNA-抗体的相互作用,以研究结合的动力学方面,并通过圆二色谱法研究结合后的构象变化。用结合位点螯合测定法分析选择的RNA,并显示出与铁蛋白竞争结合抗原结合位点。此处描述的实验表明,强结构限制的引入不必干扰选择紧密且特异性结合的RNA分子的能力。

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