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Innovative qPCR using interfacial effects to enable low threshold cycle detection and inhibition relief

机译:创新的qPCR利用界面效应实现低阈值循环检测和抑制缓解

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Molecular diagnostics offers quick access to information but fails to operate at a speed required for clinical decision-making. Our novel methodology, droplet-on-thermocouple silhouette real-time polymerase chain reaction (DOTS qPCR), uses interfacial effects for droplet actuation, inhibition relief, and amplification sensing. DOTS qPCR has sample-to-answer times as short as 3 min 30 s. In infective endocarditis diagnosis, DOTS qPCR demonstrates reproducibility, differentiation of antibiotic susceptibility, subpicogram limit of detection, and thermocycling speeds of up to 28 s/cycle in the presence of tissue contaminants. Langmuir and Gibbs adsorption isotherms are used to describe the decreasing interfacial tension upon amplification. Moreover, a log-linear relationship with low threshold cycles is presented for real-time quantification by imaging the droplet-on-thermocouple silhouette with a smartphone. DOTS qPCR resolves several limitations of commercially available real-time PCR systems, which rely on fluorescence detection, have substantially higher threshold cycles, and require expensive optical components and extensive sample preparation. Due to the advantages of low threshold cycle detection, we anticipate extending this technology to biological research applications such as single cell, single nucleus, and single DNA molecule analyses. Our work is the first demonstrated use of interfacial effects for sensing reaction progress, and it will enable point-of-care molecular diagnosis of infections.
机译:分子诊断可以快速访问信息,但无法以临床决策所需的速度运行。我们的新颖方法,即液滴对热电偶的轮廓实时聚合酶链反应(DOTS qPCR),利用界面效应来实现液滴驱动,抑制缓解和扩增传感。 DOTS qPCR的从样品到答案的时间短至3分钟30 s。在感染性心内膜炎的诊断中,DOTS qPCR表现出可重现性,抗生素敏感性的区分,亚皮克检测限以及在存在组织污染物的情况下高达28 s /循环的热循环速度。 Langmuir和Gibbs吸附等温线用于描述扩增时界面张力的降低。此外,通过使用智能手机对液滴对热电偶的轮廓进行成像,提出了具有低阈值周期的对数线性关系以进行实时定量。 DOTS qPCR解决了市售实时PCR系统的一些局限性,这些局限性依赖于荧光检测,阈值周期高得多,并且需要昂贵的光学组件和大量样品制备。由于低阈值循环检测的优势,我们期望将该技术扩展到生物学研究应用,例如单细胞,单核和单DNA分子分析。我们的工作是首次证明使用界面效应来感应反应进程,并且它将使感染的现场护理分子诊断成为可能。

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