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Lipid modified polymers for transfection of human CRL fibroblasts, and for siRNA mediated MDR reversal in melanoma cancer therapy.

机译:脂质修饰的聚合物,用于转染人类CRL成纤维细胞,以及用于黑色素瘤癌症治疗中siRNA介导的MDR逆转。

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摘要

Gene delivery for therapeutic purposes is quickly emerging as the best potential treatment option for inherited genetic diseases and cancer. Viral gene carriers have been the choice for this purpose due to their high efficiency, but harmful immunogenic and oncogenic host reactions have limited their in vivo use. Cationic polymers provide a safe alternative to viral carriers as they can be engineered to reduce immunogenic and toxic responses and serve therapeutic purposes in the body. Due to their strong positive charge, they are able to compact the negatively charged nucleotides to small nano-sized particles appropriate for cellular uptake. Additionally, they efficiently encapsulate the highly sensitive nucleotides, and protect them against degradation by the nucleases present at the physiological milieu. In this thesis work, I have used a novel approach for gene delivery by combining the critical properties of a cationic polymer (i.e., nucleotide condensing ability) with that of a fatty acid (i.e., lipid membrane compatibility). The resulting lipid modified polymer increased delivery of our gene of interest into target cells and resulted in increased siRNA delivery for gene therapy.
机译:用于治疗目的的基因递送正在迅速成为遗传性疾病和癌症的最佳潜在治疗选择。病毒基因载体由于其高效率而已成为该目的的选择,但是有害的免疫原性和致癌宿主反应限制了它们的体内使用。阳离子聚合物可作为病毒载体的安全替代品,因为可以对其进行改造以减少免疫原性和毒性反应并在体内发挥治疗作用。由于它们的强正电荷,它们能够将带负电荷的核苷酸压缩为适合细胞摄取的纳米尺寸的小颗粒。另外,它们有效地封装了高度敏感的核苷酸,并保护它们免受生理环境中存在的核酸酶降解。在本论文中,我通过结合阳离子聚合物的关键特性(即核苷酸缩合能力)和脂肪酸的关键特性(即脂质膜相容性),使用了一种新颖的基因传递方法。所得的脂质修饰的聚合物增加了我们感兴趣的基因向靶细胞的传递,并导致基因治疗的siRNA传递增加。

著录项

  • 作者

    Abbasi, Meysam.;

  • 作者单位

    University of Alberta (Canada).;

  • 授予单位 University of Alberta (Canada).;
  • 学科 Engineering Biomedical.
  • 学位 Ph.D.
  • 年度 2010
  • 页码 237 p.
  • 总页数 237
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 老年病学;
  • 关键词

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