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A Focused Poly(Aminoether) Library for Transgene Delivery to Cancer Cells.

机译:聚焦聚(氨基醚)文库,用于将基因转移至癌细胞。

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摘要

Cancer diseases are among the leading cause of death in the United States. Advanced cancer diseases are characterized by genetic defects resulting in uncontrollable cell growth. Currently, chemotherapeutics are one of the mainstream treatments administered to cancer patients but are less effective if administered in the later stages of metastasis, and can result in unwanted side effects and broad toxicities. Therefore, current efforts have explored gene therapy as an alternative strategy to correct the genetic defects associated with cancer diseases, by administering genes which encode for proteins that result in cell death. While the use of viral vectors shows high level expression of the delivered transgene, the potential for insertion mutagenesis and activation of immune responses raise concern in clinical applications. Non-viral vectors, including cationic lipids and polymers, have been explored as potentially safer alternatives to viral delivery systems. These systems are advantageous for transgene delivery due to ease of synthesis, scale up, versatility, and in some cases due to their biodegradability and biocompatibility. However, low efficacies for transgene expression and high cytotoxicities limit the practical use of these polymers.;In this work, a small library of twenty-one cationic polymers was synthesized following a ring opening polymerization of diglycidyl ethers (epoxides) by polyamines. The polymers were screened in parallel and transfection efficacies of individual polymers were compared to those of polyethylenimine (PEI), a current standard for polymer-mediated transgene delivery. Seven lead polymers that demonstrated higher transgene expression efficacies than PEI in pancreatic and prostate cancer cells lines were identified from the screening. A second related effort involved the generation of polymer-antibody conjugates in order to facilitate targeting of delivered plasmid DNA selectively to cancer cells. Future work with the novel lead polymers and polymer-antibody conjugates developed in this research will involve an investigation into the delivery of transgenes encoding for apoptosis-inducing proteins both in vitro and in vivo.
机译:癌症疾病是美国主要的死亡原因之一。晚期癌症疾病的特征是遗传缺陷导致细胞无法控制的生长。当前,化学疗法是向癌症患者施用的主流疗法之一,但是如果在转移的后期阶段施用则效果较差,并且可能导致不良的副作用和广泛的毒性。因此,当前的努力已经探索了基因疗法,作为通过施用编码导致细胞死亡的蛋白质的基因来纠正与癌症疾病相关的遗传缺陷的替代策略。尽管病毒载体的使用显示了所传递的转基因的高水平表达,但是插入诱变和免疫应答激活的潜力在临床应用中引起关注。已经研究了包括阳离子脂质和聚合物在内的非病毒载体,作为病毒传递系统的潜在安全替代品。这些系统由于易于合成,规模化,多功能性以及在某些情况下由于其生物降解性和生物相容性而有利于转基因递送。然而,转基因表达的低效率和高细胞毒性限制了这些聚合物的实际应用。在这项工作中,在二胺缩水甘油醚(环氧化物)通过多胺开环聚合后,合成了一个小的二十一阳离子聚合物库。平行筛选聚合物,并将单个聚合物的转染效率与聚乙烯亚胺(PEI)的转染效率进行比较,PEI是聚合物介导的转基因递送的当前标准。从筛选中鉴定出七个在胰腺和前列腺癌细胞系中表现出比PEI更高的转基因表达效率的先导聚合物。第二相关的工作涉及聚合物-抗体缀合物的产生,以便于将递送的质粒DNA选择性地靶向癌细胞。这项研究中开发的新型先导聚合物和聚合物-抗体结合物的未来工作将涉及在体外和体内对编码凋亡诱导蛋白的转基因的传递进行研究。

著录项

  • 作者

    Vu, Lucas.;

  • 作者单位

    Arizona State University.;

  • 授予单位 Arizona State University.;
  • 学科 Engineering Biomedical.;Health Sciences Oncology.;Engineering Chemical.
  • 学位 M.S.
  • 年度 2011
  • 页码 71 p.
  • 总页数 71
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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