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Study and development of label-free optical biosensors for biomedical applications

机译:研究和开发用于生物医学应用的无标记光学生物传感器

摘要

For the majority of assays currently performed, fluorescent or colorimetric chemical labels are commonly attached to the molecules under study so that they may be readily visualized. The methods of using labels to track biomolecular binding events are very sensitive and effective, and are employed as standardized assay protocol across research labs worldwide. However, using labels induces experimental uncertainties due to the effect of the label on molecular conformation, active binding sites, or inability to find an appropriate label that functions equivalently for all molecules in an experiment. Therefore, the ability to perform highly sensitive biochemical detection without the use of fluorescent labels would further simplify assay protocols and would provide quantitative kinetic data, while removing experimental artifacts from fluorescent quenching, shelf-life, and background fluorescence phenomena. In view of the advantages mentioned above, the study and development of optical label-free sensor technologies have been undertaken here. In general, label-free photonic crystal (PC) biosensors and metal nanodome array surface-enhanced Raman scattering (SERS) substrates, both of which are fabricated by nanoreplica molding process, have been used as the method to attack the problem. Chapter 1 shows the work on PC label-free biosensor incorporated microfluidic network for bioassay performance enhancement and kinetic reaction rate constant determination. Chapter 2 describes the work on theoretical and experimental comparison of label-free biosensing in microplate, microfluidic, and spot-based affinity capture assays. Chapter 3 shows the work on integration of PC biosensor with actuate-to-open valve microfluidic chip for pL-volume combinatorial mixing and screening application. In Chapter 4, the development and characterization of SERS nanodome array is shown. Lastly, Chapter 5 describes SERS nanodome sensor incorporated tubing for point-of-care monitoring of intravenous drugs and metabolites.
机译:对于当前执行的大多数测定,通常将荧光或比色化学标记附着在研究的分子上,以便可以轻松看到它们。使用标记追踪生物分子结合事件的方法非常敏感和有效,并且已被全世界的研究实验室用作标准化测定方案。但是,由于标记对分子构象,活性结合位点的影响或无法找到对实验中所有分子均具有等效功能的适当标记,因此使用标记会引起实验不确定性。因此,在不使用荧光标记的情况下进行高度灵敏的生化检测的能力将进一步简化测定方案,并提供定量动力学数据,同时从荧光猝灭,保质期和背景荧光现象中去除实验假象。鉴于上述优点,这里已经进行了无标签光学传感器技术的研究和开发。通常,无标签的光子晶体(PC)生物传感器和金属纳米球阵列表面增强拉曼散射(SERS)基板,都是通过纳米复制模制工艺制造的,已被用作解决该问题的方法。第1章介绍了结合了微流体网络的无PC标签生物传感器的工作,该生物流体用于增强生物测定性能和动力学反应速率常数。第2章介绍了在微孔板,微流控和基于斑点的亲和捕获测定中无标记生物传感的理论和实验比较的工作。第三章介绍了将PC生物传感器与驱动开阀微流体芯片集成在一起的工作,以进行pL体积组合混合和筛选应用。在第四章中,展示了SERS纳米球阵列的开发和表征。最后,第5章介绍了内置有SERS纳米球传感器的管道,用于即时监测静脉内药物和代谢产物。

著录项

  • 作者

    Choi Charles J.;

  • 作者单位
  • 年度 2011
  • 总页数
  • 原文格式 PDF
  • 正文语种 {"code":"en","name":"English","id":9}
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