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Technologies for Protein Analysis and Tissue Engineering, with Applications in Cancer.

机译:蛋白质分析和组织工程技术及其在癌症中的应用。

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摘要

The first part of this thesis describes electrolyte transport through an array of 20 nm wide, 20 mum long SiO2 nanofluidic transistors. At sufficiently low ionic strength, the Debye screening length exceeds the channel width, and ion transport is limited by the negatively charged channel surfaces. At source-drain biases > 5 V, the current exhibits a sharp, nonlinear increase, with a 20 - 50-fold conductance enhancement. This behavior is attributed to a breakdown of the zero-slip condition. Implications for peptide sequencing as well as energy conversion devices are discussed.;The next part describes a technology for the detection of the highly aggressive brain cancer glioblastoma multiforme (GBM). In this study, we used an antibody-based microarray to compare plasma samples from glioblastoma patients and healthy controls with respect to the plasma levels of 35 different proteins known to be generally associated with tumor growth, survival, invasion, migration, and immune regulation. Average-linkage hierarchical clustering of the patient data stratified the two groups effectively, permitting accurate assignment of test samples into either GBM or healthy control groups with a sensitivity and specificity as high as 90 % and 94 %, respectively. Using the same 35-protein panel, we then analyzed plasma samples from GBM patients who were treated with the chemotherapeutic drug Avastin (Bevacizumab) and were able to effectively stratify patients based on treatment-responsiveness. Finally, single-cell resolution patterning of tissue engineered structures is demonstrated. The proper functioning of engineered constructs for tissue and organ transplantation requires positioning different cell types in anatomically precise arrangements that mimic their configurations in native tissues. Toward this end, we have developed a technique that involves two microfluidic-patterning steps run perpendicularly to each other using "anchor" and "bridge" DNA oligomers to create dense arrays of DNA grids which can then be converted into cell arrays. As a proof-of-concept, both a neuron-astrocyte construct and a pancreatic islet construct containing 2 distinct islet cell types were patterned separately as a dense array of cell grids. Once fixed in a hydrogel matrix, layers of patterned cells were then stacked to form 3-D tissue engineered constructs.
机译:本文的第一部分描述了电解质通过20纳米宽,20微米长的SiO2纳米流体晶体管阵列的传输。在足够低的离子强度下,德拜屏蔽长度超过了通道宽度,并且离子传输受到带负电荷的通道表面的限制。在源极-漏极偏置> 5 V时,电流呈现出急剧的非线性增加,电导提高20至50倍。此行为归因于零滑移条件的故障。讨论了肽测序以及能量转换装置的意义。下一部分描述了一种用于检测高度侵袭性脑癌多形胶质母细胞瘤(GBM)的技术。在这项研究中,我们使用了一种基于抗体的微阵列来比较胶质母细胞瘤患者和健康对照者的血浆样品中35种不同蛋白质的血浆水平,这些蛋白质通常与肿瘤的生长,存活,侵袭,迁移和免疫调节有关。患者数据的平均链接层次聚类有效地将两组进行了分层,从而可以将测试样品准确地分配到GBM或健康对照组中,敏感性和特异性分别高达90%和94%。然后,使用相同的35种蛋白质组,我们分析了使用化疗药物Avastin(Bevacizumab)治疗的GBM患者的血浆样品,这些患者能够根据治疗反应有效地对患者进行分层。最后,演示了组织工程结构的单细胞分辨率模式。用于组织和器官移植的工程构建体的正常功能需要以解剖学精确的排列方式定位不同的细胞类型,以模仿其在天然组织中的构型。为此,我们开发了一种技术,该技术涉及使用“锚”和“桥” DNA寡聚物彼此垂直运行的两个微流控图案化步骤,以创建致密的DNA网格阵列,然后将其转化为细胞阵列。作为概念验证,神经元-星形细胞构建体和包含2种不同胰岛细胞类型的胰岛构建体都被分别图案化为密集的细胞网格阵列。一旦固定在水凝胶基质中,然后将图案化细胞层堆叠以形成3-D组织工程化构建体。

著录项

  • 作者

    Vermesh, Udi Benjamin.;

  • 作者单位

    California Institute of Technology.;

  • 授予单位 California Institute of Technology.;
  • 学科 Biomedical engineering.;Oncology.;Biochemistry.;Nanotechnology.
  • 学位 Ph.D.
  • 年度 2011
  • 页码 151 p.
  • 总页数 151
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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