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NIR-emissive polymersomal markers for molecular-level detection of metastasis.

机译:近红外发射多聚体标记物,用于转移水平的分子检测。

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摘要

Noninvasive imaging technologies, capable of visualizing early carcinoma or dormant or latent metastatic tumor cells and evaluating the efficacy of cancer therapies are becoming increasingly important. In this thesis, NIR-emissive polymersomes are engineered for optimal cellular uptake to enable fluorescence-based tumor targeting. A series of benzothiadiazole conjugated porphyrin oligomers with high emission dipole strength and exceptional large quantum yields in the NIR region are synthesized for optimized emissive output would be greatly enhanced. Furthermore, this thesis established for the first time a class of universal chemistry modification methods to directly attach antibody to polymersomes surface with very high antibody coupling efficiency and precise control of antibody density on polymersomes. These antibody conjugated NIR-emissive polymersomes exhibit ideal cell-surface adhesion dynamics and enables future in vivo tracking of labeled tumor cells by NIR fluorescence based imaging.;Ultimately, tracking residual disease in vivo requires biodegradable polymersomes. Towards this goal, we fabricated analogous nanoscale NIR-emissive, soft-matter-based vesicles based on already FDA-approved materials poly(caprolactone) (PCL) and poly(trimethylene carbonate) (PTMC) blocks, and involves copolymer synthesis, evaluation of vesicle physical properties, and polymersome functionalization. Finally, a new emissive polymersomes platform is designed by quantitative incorporation of quantum dots into the polymersomes bilayer membranes, featuring a wide range of applications for in vivo diagnostic and drug-delivery applications.;In summary, this synthesis developed functionalized nanoscale NIR-emissive polymersomes with optimal fluorescence output and ability to detect limited target cell numbers under clinically relevant diagnostic conditions, and define new tools for the study of metastatic disease.
机译:能够可视化早期癌症,休眠或潜在转移性肿瘤细胞并评估癌症治疗效果的非侵入性成像技术变得越来越重要。在这篇论文中,近红外发射聚合物囊泡经过工程改造,可实现最佳的细胞摄取,从而实现基于荧光的肿瘤靶向。合成了一系列在NIR区域具有高发射偶极强度和超大量子产率的苯并噻二唑共轭卟啉低聚物,可大大提高优化的发射功率。此外,本论文首次建立了一类通用的化学修饰方法,以非常高的抗体偶联效率和精确控制多核小体上的抗体密度直接将抗体附着于多核小体表面。这些结合了抗体的NIR发射聚合物囊泡表现出理想的细胞表面粘附动力学,并能够通过基于NIR荧光的成像在体内进行标记肿瘤细胞的未来跟踪。最终,跟踪体内残留的疾病需要可生物降解的聚合物囊泡。为了实现这一目标,我们基于已经获得FDA批准的材料聚己内酯(PCL)和聚碳酸三亚甲基酯(PTMC)嵌段,制造了类似的基于NIR发射,基于软物质的纳米囊泡,涉及共聚物的合成,囊泡的物理性质和多聚体功能化。最后,通过将量子点定量掺入聚合物囊泡双层膜中,设计了一个新的发射聚合物囊泡平台,该平台具有广泛的体内诊断和药物递送应用领域。总之,该合成开发了功能化的纳米级近红外发射聚合物囊泡。具有最佳的荧光输出能力,并能够在临床相关的诊断条件下检测有限的靶细胞数量,并为研究转移性疾病定义了新的工具。

著录项

  • 作者

    Qi, Wei.;

  • 作者单位

    University of Pennsylvania.;

  • 授予单位 University of Pennsylvania.;
  • 学科 Chemistry Analytical.;Chemistry Polymer.;Chemistry Organic.
  • 学位 Ph.D.
  • 年度 2011
  • 页码 339 p.
  • 总页数 339
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

  • 入库时间 2022-08-17 11:45:19

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