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Synthesis of two novel grafted polyethylenimines for enhanced delivery of biologically active agents to mammalian cells.

机译:两种新型接枝聚乙烯亚胺的合成,用于增强生物活性剂向哺乳动物细胞的递送。

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摘要

Delivery of fragile, biologically active substances is of increasing interest in the treatment of various disease states. For three decades, drug delivery has focused on long-term cases (i.e. localized delivery to a tumor), or targeted delivery (i.e. a selected cell type). The next horizon falls into intracellular delivery (e.g. delivery of the drug to the appropriate intracellular compartment). For several years polyethylenimine (PEI) has been used as a non-viral means of delivering DNA to cells. Polymeric systems have many theoretical advantages compared with other non-viral delivery techniques (e.g. liposomes). PEI, however, has failed to produce high transfection levels as anticipated. We have developed two modified PEI complexes for the delivery of biologically active substances to cells. These modifications retain the attractive properties of native PEI, but address possible shortcomings discovered with DNA delivery observed by many groups. Our modifications consist of grafting low molecular weight, branched form PEI together into a large complex, wherein the linkages can be cleaved by intracellular machinery. Proteins can be linked to the novel PEI complexes through the establishment of a disulfide bond, thereby expanding the utility of PEI as a delivery system. Intracellular delivery is then accomplished by reducing agents within the cytosol of the cell, thus effecting protein delivery to cells. Using the novel grafted PEI molecules, we have successfully protected and delivered biologically active proteins and DNA to targeted cells.
机译:脆弱的生物活性物质的递送在各种疾病状态的治疗中越来越受到关注。三十年来,药物递送一直集中于长期病例(即局部递送至肿瘤)或靶向递送(即选定的细胞类型)。下一个视野落入细胞内递送(例如,将药物递送至适当的细胞内区室)。几年来,聚乙烯亚胺(PEI)被用作将DNA传递到细胞的非病毒手段。与其他非病毒递送技术(例如脂质体)相比,聚合物系统具有许多理论优势。但是,PEI无法产生预期的高转染水平。我们已经开发了两种修饰的PEI复合物,用于将生物活性物质输送至细胞。这些修饰保留了天然PEI的吸引人的特性,但解决了许多团体观察到的DNA传递所发现的可能缺点。我们的修饰包括将低分子量,支链形式的PEI嫁接到一个大的复合物中,其中的连接可以通过细胞内机制进行切割。蛋白质可以通过建立二硫键与新型PEI复合物相连,从而扩大了PEI作为递送系统的用途。然后通过还原细胞胞质内的试剂完成细胞内传递,从而实现蛋白质向细胞的传递。使用新型的接枝PEI分子,我们已经成功地保护了具有生物活性的蛋白质和DNA并将其传递至目标细胞。

著录项

  • 作者

    Braden, Arthur Robert Coe.;

  • 作者单位

    The University of Texas at Arlington.;

  • 授予单位 The University of Texas at Arlington.;
  • 学科 Engineering Biomedical.; Health Sciences Pharmacology.
  • 学位 Ph.D.
  • 年度 2003
  • 页码 143 p.
  • 总页数 143
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 生物医学工程;药理学;
  • 关键词

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