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Biophysical investigations of boranophosphate siRNA for use in RNA interference against human disease.

机译:用于干扰人类疾病的RNA干扰的硼磷酸siRNA的生物物理研究。

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摘要

This project is predicated on the ability of the boranophosphate modification of siRNA to increase its therapeutic applicability for gene silencing in in vitro and in vivo systems. It has been shown that the boranophosphate (BH3-PO3) can overcome many of the limitations that are traditionally found when using RNAi, namely nuclease stability. The synthesis of siRNA modified with 5'-(alpha-P-borano)-nucleoside triphosphates (NTP) analogs alone and in combination with 2'-deoxy-2'-fluoro nucleoside triphosphate analogs were performed and optimized. It was found that normal RNA transcriptions showed the highest yield with higher NTP concentrations and shorter incubation times. Boranophosphate modified RNA and 2'F/borano modified RNA transcription yield was optimal at lower NTP concentrations and extended incubations. The boranophosphate NTPs and RNA were characterized with high performance liquid chromatography, mass spectrometry, and nuclear magnetic resonance, indicating successful synthesis of NTPalphaB and 2'F NTPs. PAGE and mass spectrometry analysis were performed to ensure full-length transcription of the modified siRNA molecules. The effects of these modifications were explored with respect to the biophysical properties of the modified homoduplex and heteroduplex siRNA. The techniques used in this work included hybridization affinity assays (melting temperature), secondary structure determination (circular dichroism), nuclease stability assays, and assessment of the lipophilicity of the modified siRNA by determining partition coefficients.;Modification of siRNA with boranophosphate and 2'fluoro/borano modified NTPs appears to have caused the homoduplexes and heteroduplexes to adopt a more B form-like helix that had lower Tm compared to unmodified RNA. The stability of the siRNA transcript to enzymatic hydrolysis by Exonuclease T was on the order of 2'fluoro/borano> normal = boranophosphate. Boranophosphate modification increased the stability of the transcript to enzymatic hydrolysis by the endonuclease RNase A, compared to both normal and 2' fluoro modified siRNA. Overall, the 2' fluoro/borano modified siRNA showed the greatest biological stability. Modification of the siRNA with increasing percentages of boranophosphates resulted in increasing lipophilicity of the molecule up to 60-fold, compared to both normal and 2' fluoro RNA.;A method to site-specifically modify the boranophosphate siRNA using T4 RNA ligase was also investigated. Finally, the siRNA in this work was tested in several in vitro systems, yielding promising results for the usage of boranophosphate siRNA for use against human viruses and cancers. It was shown that in for in vitro systems for human papillomavirus gene expression (HeLa, SiHa, and W12E) and luciferase expression (B16F10 cells), boranophosphate modified siRNA can specifically downregulate gene expression, and in the case of human papillomavirus, can downregulate cell growth.
机译:该项目基于对siRNA的硼磷酸修饰的能力,以提高其在体外和体内系统中基因沉默的治疗性。已经表明,硼酸磷酸酯(BH3-PO3)可以克服使用RNAi时传统发现的许多限制,即核酸酶稳定性。单独进行了5'-(α-P-硼烷)-核苷三磷酸酯(NTP)类似物修饰的siRNA的合成,并与2'-脱氧-2'-氟核苷三磷酸酯类似物组合进行了优化。发现正常的RNA转录在较高的NTP浓度和较短的孵育时间下显示出最高的产量。硼酸磷酸酯修饰的RNA和2'F /硼酸修饰的RNA转录产量在较低的NTP浓度和延长的孵育时间下是最佳的。通过高效液相色谱,质谱和核磁共振对硼酸磷酸酯NTPs和RNA进行了表征,表明NTPalphaB和2'F NTPs的成功合成。进行PAGE和质谱分析以确保修饰的siRNA分子的全长转录。关于修饰的同源双链体和异源双链体siRNA的生物物理特性,探讨了这些修饰的作用。在这项工作中使用的技术包括杂交亲和力测定(融化温度),二级结构测定(圆二色性),核酸酶稳定性测定,以及通过确定分配系数评估修饰的siRNA的亲脂性;用硼酸磷酸酯和2'修饰siRNA。氟/硼烷修饰的NTPs似乎导致同双链体和异双链体采用了更多的B型螺旋,其Tm低于未修饰的RNA。 siRNA转录物对核酸外切酶T的酶促水解的稳定性大约为2'氟/硼烷>正常=硼磷酸。与正常和2'氟修饰的siRNA相比,硼酸磷酸酯修饰增加了转录本对内切酶RNase A进行酶水解的稳定性。总体而言,2'氟/硼烷修饰的siRNA表现出最大的生物学稳定性。与正常和2'氟RNA相比,随着硼酸磷酸酯百分比的增加而对siRNA进行的修饰导致分子的亲脂性增加高达60倍。;还研究了使用T4 RNA连接酶定点修饰硼酸磷酸siRNA的方法。最后,这项工作中的siRNA在多个体外系统中进行了测试,使用硼酸磷酸siRNA对抗人类病毒和癌症产生了可喜的结果。结果表明,在人乳头瘤病毒基因表达(HeLa,SiHa和W12E)和萤光素酶表达(B16F10细胞)的体外系统中,硼磷酸修饰的siRNA可以特异性地下调基因表达,而在人乳头瘤病毒的情况下,可以下调细胞增长。

著录项

  • 作者

    Moussa, Laura W.;

  • 作者单位

    Duke University.;

  • 授予单位 Duke University.;
  • 学科 Chemistry Biochemistry.
  • 学位 Ph.D.
  • 年度 2009
  • 页码 237 p.
  • 总页数 237
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 生物化学;
  • 关键词

  • 入库时间 2022-08-17 11:37:42

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