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Multilayered Nanoplasmonic Arrays for Self-Referenced Biosensing

机译:用于自我引用的生物传感的多层纳米型阵列

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Nanostructured sensors based on localized surface plasmon resonance (LSPR) offer a number of advantages over other optical sensing technologies, making them excellent candidates for miniaturized, label-free chemical and biological detection. Highly sensitive to local refractive index changes, the resonance peaks of the nanosensors shift by different amounts when subject to different biological and chemical environments. Modifications to the nanostructure surface allow for the detection of specific molecules and chemicals with shifts so sensitive that the presence of single molecules can be detected. However, this extreme sensitivity has its drawbacks. Resonance shifts also occur because of temperature shifts, light-intensity fluctuations, and other environmental factors. To distinguish detection from drift, a secondary sensor region is often required. This often doubles the size of the device, requires two light sources and detectors (or complex optics), doubles the sample volume required (which may be expensive, or may not be possible if the sample quantity is limited), and subjects the reference to potential biofouling. Here, we present a new proof-of-concept multilayered LSPR sensor design that incorporates both a sensing layer and an encapsulated reference layer within the same region. By doing so, we are able to monitor and correct for sensor drift without the need for a secondary reference channel. We demonstrate the suitability of this sensor for sucrose concentration measurements and for the detection of biotin-avidin interactions, while also showing that the sensor can self-correct for drift. We believe that this multilayer sensor design holds promise for point-of-care diagnostics.
机译:基于局部表面等离子体谐振(LSPR)的纳米结构传感器提供了许多优于其他光学传感技术的优势,使其成为小型化,无标记化学和生物检测的优异候选者。对局部折射率的高度敏感,纳米传感器的共振峰在受不同的生物和化学环境受到不同的情况下偏移不同的量。对纳米结构表面的修饰允许检测特定分子和化学物质的变化如此敏感,即可以检测单个分子的存在。然而,这种极端敏感性具有其缺点。由于温度偏移,光强度波动和其他环境因素,共振移位也会发生。为了区分从漂移的检测,通常需要辅助传感器区域。这通常使装置的尺寸加倍,需要两个光源和探测器(或复杂的光学器件),加倍所需的样品体积(如果样品量有限),则可能是不可能的,或者可能是不可能的,并且对其进行参考潜在的生物污染。在这里,我们提出了一种新的概念证明多层LSPR传感器设计,其包括同一区域内的感测层和封装的参考层。通过这样做,我们能够监控和更正传感器漂移,而无需辅助参考通道。我们证明了该传感器对蔗糖浓度测量和检测生物素 - 抗生物素蛋白相互作用的适用性,同时还表明传感器可以自校正漂移。我们认为,这种多层传感器设计能够对护理点诊断提供承担。

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