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Analytical chemistry at the interface between materials science and biology.

机译:材料科学与生物学之间的交界处的分析化学。

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摘要

This work describes several research efforts that lie at the new interfaces between analytical chemistry and other disciplines, namely materials science and biology. In the materials science realm, the search for new materials that may have useful or unique chromatographic properties motivated the synthesis and characterization of electrically conductive sol-gels. In the biology realm, the search for new surface fabrication schemes that would permit or even improve the detection of specific biological reactions motivated the design of miniaturized biological arrays. Collectively, this work represents some of analytical chemistry's newest forays into these disciplines.; This dissertation is divided into six chapters. Chapter 1 is an introductory chapter that provides background information pertinent to several key aspects of the work contained in this dissertation. Chapter 2 describes the synthesis and characterization of electrically conductive sol-gels derived from the acid-catalyzed hydrolysis of a vanadium alkoxide. Specifically, this chapter describes our attempts to increase the conductivity of vanadium sol-gels by optimizing the acidic and drying conditions used during synthesis. Chapter 3 reports the construction of novel antigenic immunosensing platforms of increased epitope density using Fab-SH antibody fragments on gold. Here, X-ray photoelectron spectroscopy (XPS), thin-layer cell (TLC) and confocal fluorescence spectroscopies, and scanning force microscopy (SFM) are employed to characterize the fragment-substrate interaction, to quantify epitope density, and to demonstrate fragment viability and specificity. Chapter 4 presents a novel method for creating and interrogating double-stranded DNA (dsDNA) microarrays suitable for screening protein:dsDNA interactions. Using the restriction enzyme ECoR1, we demonstrate the ability of the atomic force microscope (AFM) to detect changes in topography that result from the enzymatic cleavage of dsDNA microarrays containing the correct recognition sequence. Chapter 5 explores more fully the microarray fabrication process described in Chapter 4. Specifically, experiments characterizing the effect of deposition conditions on oligonucleotide topography and as well as those that describe array density optimization are presented. Chapter 6 presents general conclusions from the work recorded in this dissertation and speculates on its extension.
机译:这项工作描述了位于分析化学与其他学科(即材料科学和生物学)之间的新接口的多项研究成果。在材料科学领域,对可能具有有用或独特色谱特性的新材料的探索促进了导电溶胶凝胶的合成和表征。在生物学领域,寻找将允许甚至改善对特定生物反应的检测的新表面制造方案的探索,促使了小型化生物阵列的设计。总的来说,这项工作代表了分析化学在这些学科领域的最新尝试。本文共分为六章。第1章是绪论性的一章,提供了与本文所涉及工作的几个关键方面有关的背景信息。第2章介绍了由酸催化的钒醇盐水解得到的导电溶胶-凝胶的合成和表征。具体而言,本章介绍了我们通过优化合成过程中使用的酸性和干燥条件来提高钒溶胶凝胶电导率的尝试。第三章报道了在金上使用Fab ' -SH抗体片段构建表位密度增加的新型抗原免疫传感平台的方法。在这里,使用X射线光电子能谱(XPS),薄层细胞(TLC)和共聚焦荧光光谱仪以及扫描力显微镜(SFM)来表征片段与底物的相互作用,定量表位密度,并展示片段的活力和特异性。第4章介绍了一种新颖的方法,用于创建和询问适合筛选蛋白质:dsDNA相互作用的双链DNA(dsDNA)微阵列。使用限制酶 ECo R1,我们证明了原子力显微镜(AFM)检测包含正确识别序列的dsDNA微阵列的酶切作用引起的拓扑变化的能力。第5章更加全面地探讨了第4章中描述的微阵列制造过程。具体而言,提出了表征沉积条件对寡核苷酸形貌的影响的实验以及描述阵列密度优化的实验。第六章给出了本文所记录工作的一般结论,并推测了其扩展性。

著录项

  • 作者

    O'Brien, Janese Christine.;

  • 作者单位

    Iowa State University.;

  • 授予单位 Iowa State University.;
  • 学科 Chemistry Analytical.; Engineering Materials Science.; Chemistry Biochemistry.
  • 学位 Ph.D.
  • 年度 2000
  • 页码 119 p.
  • 总页数 119
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 化学;工程材料学;生物化学;
  • 关键词

  • 入库时间 2022-08-17 11:47:52

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