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Digital-microfluidic biochips for quantitative analysis: Bridging the Gap between microfluidics and microbiology

机译:数码微流体生物芯片用于定量分析:桥接微流体和微生物学之间的差距

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Digital-microfluidics technology has shown considerable promise for advancing sample preparation and point-of-care diagnostics; therefore, it has the potential to transform microbiology and biochemistry research. Over the past decade, a number of microfluidics design-automation techniques have been developed for on-chip droplet manipulation. However, these methods overlook the myriad complexities of biomolecular protocols and they have yet to make a significant impact in biochemistry/microbiology research. A paradigm shift in biochip design automation and a “phase transition” in research are clearly needed to bridge this gap between microfluidics and microbiology. In this paper, we explain how researchers from design-automation and embedded systems can play a key role in this transition. We present a new synthesis flow that uses realistic models of biomolecular protocols and cyberphysical adaptation to address real-world microbiology applications. We also present a list of metrics that can be used for the assessment of designautomation techniques for microbiology applications.
机译:数字微流体技术对推进样品准备和护理点诊断表现出相当大的承诺;因此,它有可能转化微生物学和生物化学研究。在过去十年中,已经开发了许多微流体设计 - 自动化技术,用于片上液滴操作。然而,这些方法忽略了生物分子方案的无数复杂性,并且他们尚未对生物化学/微生物学研究产生重大影响。显然需要在生物芯片设计自动化和“相位过渡”中的范式转变,以弥合微流体和微生物学之间的这种差距。在本文中,我们解释了研究人员如何从设计 - 自动化和嵌入式系统中发挥这种转变中的关键作用。我们介绍了一种新的合成流程,使用生物分子协议和控制器适应的现实模型来解决现实世界微生物学应用。我们还提供了一份可用于评估微生物学应用的设计的指标列表。

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