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Single-Molecule Topochemical Analyses for Large-Scale Multiplexing Tasks

机译:用于大规模复用任务的单分子TopeChemical分析

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摘要

Multitasking is the pivotal feature in next-generation chemo- or bioanalyses. However, simultaneous analyses rarely exceed over three different tasks, which is ascribed to the limited space to accommodate analyzing units and the compromised signal-to-noise (S/N) level as the number of tasks increases. Here, by leveraging superior S/N of single-molecule techniques, we analyzed five microRNA biomarkers by spatially encoding miRNA recognition units with nanometers resolution in a DNA template, while decoding the analyte binding temporally in seconds. The hairpin stem is interspersed by internal loops to encode recognition units for miRNA. By mechanical unfolding of the hairpin, individual internal loops are sequentially interrogated for the binding of each miRNA. Using this so-called topochemical spatiotemporal analysis, we were able to achieve subpicomolar detection limits of miRNAs. We anticipate that this new single-molecule topochemical analysis can massively analyze single-molecule targets.
机译:多任务处理是下一代化学或生物甘露体内的关键特征。然而,同时分析很少超过三种不同的任务,其归因于有限的空间,以适应分析单元和随着任务数量的增加而受损的信号对噪声(S / N)水平。这里,通过利用单分子技术的上生S / N,通过在DNA模板中空间编码miRNA识别单元来分析五个microRNA生物标志物,同时以秒为单位在时间上解码分析物结合的分析物结合。发夹杆通过内部环散射,以编码miRNA的识别单元。通过发夹的机械展开,依次询问单个内部环以询问每个miRNA的结合。使用这种所谓的Topechemical Spatiberemporal分析,我们能够实现miRNA的亚皮质摩尔检测限局限。我们预期这种新的单分子Topechemical分析可以大量分析单分子靶标。

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