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Enhancing enzymatic efficiency by attachment to semiconductor nanoparticles for biosensor applications

机译:通过附着在生物传感器应用中的半导体纳米颗粒上来提高酶促效率

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摘要

Nanosensors employing quantum dots (QDs) with appended biofunctional moieties offer tremendous promise for disease surveillance/diagnostics and chemical/biological threat activity. Their small size permits cell penetration and their inherent photochemical properties are well-suited for rapid, optical measurement. The effectiveness of enzymes immobilized on QDs, however, are not completely understood, hindering development of chemical/biological sensors and remediation materials. Here, we analyze enzyme effectiveness for the neutralization of a simulant nerve agent when attached to two distinctly-sized QDs. Two sizes of QDs, 525 or 625 nm, were appended with DHLA ligands to improve aqueous stability and prevent aggregation. Various molar ratios of de novo phosphotriesterase trimer (PTE_3) were rapidly self-assembled via spontaneous metal coordination of the PTE oligohistidine tag onto the Zn~(2+)-rich QD surface. PTE catalyzes the detoxification of organophosphate pesticides (e.g, paraoxon, an analog of sarin) to p-nitrophenol whose absorbance can be measured at 405 nm. The optimal ratio of PTE_3 to 525 nm and 625 nm QD's was determined to be 12 and 24, respectively. The enhanced enzyme performance in both cases is most likely due to increased enzyme-substrate interactions from improvements in enzyme orientation, enzyme density, and substrate diffusion on or near the QD. Development of these nansosensors as optical-based biosensors (e.g., within compact microfluidic devices) may greatly improve the sensitivity of conventional biological/chemical detection schemes.
机译:使用带有附加的生物功能部分的量子点(QD)的纳米传感器为疾病监测/诊断和化学/生物威胁活动提供了广阔的前景。它们的体积小,可穿透细胞,其固有的光化学性质非常适合快速光学测量。然而,尚未完全了解固定在QD上的酶的有效性,从而阻碍了化学/生物传感器和修复材料的发展。在这里,我们分析了与两个截然不同的量子点相连时模拟神经药的中和酶的有效性。两种尺寸的525或625 nm的QD均附有DHLA配体,以改善水稳定性并防止聚集。各种摩尔比的新生磷酸三酯酶三聚体(PTE_3)通过PTE寡组氨酸标签的自发金属配位迅速富集到富含Zn〜(2+)的QD表面上。 PTE催化将有机磷酸酯农药(例如对氧磷,沙林的类似物)解毒为对硝基苯酚,对硝基苯酚的吸光度可在405 nm处测量。确定PTE_3与525 nm和625 nm QD的最佳比例分别为12和24。在这两种情况下,增强的酶性能最有可能是由于酶方向,酶密度和QD上或附近的底物扩散的改善而增加了酶与底物的相互作用。将这些纳米传感器开发为基于光学的生物传感器(例如,在紧凑的微流体装置内)可以极大地提高常规生物/化学检测方案的灵敏度。

著录项

  • 来源
  • 会议地点 Baltimore MD(US)
  • 作者单位

    Center for Bio/Molecular Science and Engineering, Code 6900 U.S. Naval Research Laboratory Washington, DC 20375,American Society for Engineering Education Washington, DC 20036;

    Center for Bio/Molecular Science and Engineering, Code 6900 U.S. Naval Research Laboratory Washington, DC 20375;

    Optical Sciences Division, Code 5600 U.S. Naval Research Laboratory Washington, DC 20375,Sotera Defense Solutions, Inc. 7230 Lee DeForest Drive Columbia, MD 21046;

    Optical Sciences Division, Code 5600 U.S. Naval Research Laboratory Washington, DC 20375,Sotera Defense Solutions, Inc. 7230 Lee DeForest Drive Columbia, MD 21046;

    Optical Sciences Division, Code 5600 U.S. Naval Research Laboratory Washington, DC 20375;

    Center for Bio/Molecular Science and Engineering, Code 6900 U.S. Naval Research Laboratory Washington, DC 20375;

    Electronic Science and Technology Division, Code 6800 U.S. Naval Research Laboratory Washington, DC 20375;

    Center for Bio/Molecular Science and Engineering, Code 6900 U.S. Naval Research Laboratory Washington, DC 20375;

  • 会议组织
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

    Quantum dots; enzyme; phopsphotriesterase; paraoxon; kinetics; biosensor;

    机译:量子点;酶磷酸三酯酶;对氧磷动力学;生物传感器;

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