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Real-time rolling circle amplification for protein detection

机译:实时滚环扩增用于蛋白质检测

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Real-time nucleic acid amplification methods can be extremely useful for the identification and quantitation of nucleic acid analytes, but are more difficult to adapt to protein or other analytes. To facilitate the development of real-time rolling circle amplification (RCA) for protein targets, we have developed a novel type of conformation-switching aptamer that can be circularized upon interaction with its protein target, the platelet-derived growth factor (PDGF). Using the structure-switching aptamer, real-time RCA can be used to specifically quantitate PDGF down to the low-nanomolar range (limit of detection, 0.4 nM), even against a background of cellular lysate. The aptamer can also be adapted to RCA on surfaces, although quantitation proved to be more difficult. One of the great advantages of the method described herein is that it can be immediately adapted to almost any aptamer and does not require two or more affinity reagents as do sandwich or proximity assays.
机译:实时核酸扩增方法对于核酸分析物的鉴定和定量非常有用,但更难以适应蛋白质或其他分析物。为了促进针对蛋白质靶标的实时滚环扩增(RCA)的开发,我们开发了一种新型的构象转换适体,可在与其蛋白质靶标(血小板衍生的生长因子)相互作用时环化。使用结构转换适体,即使在细胞裂解物的背景下,实时RCA仍可用于低至低纳摩尔范围(检测限0.4 nM)的PDGF特异性定量。适体还可以适应表面的RCA,尽管定量更困难。本文所述方法的巨大优点之一是,它可以立即适用于几乎任何适体,并且不需要像夹心法或邻近测定法那样需要两种或更多种亲和试剂。

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