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Cell-Targeted Regulation of Gene Expression through Synthetic RNA Devices.

机译:通过合成RNA装置进行细胞靶向的基因表达调控。

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摘要

The ability to interface with and program cellular function remains a challenging research frontier in biotechnology. Although the emerging field of synthetic biology has recently generated a variety of gene-regulatory strategies based on synthetic RNA molecules, few strategies exist through which to control such regulatory effects in response to specific exogenous or endogenous molecular signals. Here, we present the development of an engineered RNA-based device platform to detect and act on endogenous protein signals, linking these signals to the regulation of genes and thus cellular function.;We describe efforts to develop an RNA-based device framework for regulating endogenous genes in human cells. Previously developed RNA control devices have demonstrated programmable ligand-responsive genetic regulation in diverse cell types, and we attempted to adapt this class of cis-acting control elements to function in trans. We divided the device into two strands that reconstitute activity upon hybridization. Device function was optimized using an in vivo model system, and we found that device sequence is not as flexible as previously reported. After verifying the in vitro activity of our optimized design, we attempted to establish gene regulation in a human cell line using additional elements to direct device stability, structure, and localization. The significant limitations of our platform prevented endogenous gene regulation.;We next describe the development of a protein-responsive RNA-based regulatory platform. Employing various design strategies, we demonstrated functional devices that both up- and downregulate gene expression in response to a heterologous protein in a human cell line. The activity of our platform exceeded that of a similar, small-molecule-responsive platform. We demonstrated the ability of our devices to respond to both cytoplasmic- and nuclear-localized protein, providing insight into the mechanism of action and distinguishing our platform from previously described devices with more restrictive ligand localization requirements. Finally, we demonstrated the versatility of our device platform by developing a regulatory device that responds to an endogenous signaling protein.;The foundational tool we present here possesses unique advantages over previously described RNA-based gene-regulatory platforms. This genetically encoded technology may find future applications in the development of more effective diagnostic tools and targeted molecular therapy strategies.
机译:接口和编程细胞功能的能力仍然是生物技术领域一个具有挑战性的研究前沿。尽管合成生物学的新兴领域最近已基于合成RNA分子产生了多种基因调控策略,但很少有策略可以响应特定的外源或内源性分子信号来控制这种调控作用。在这里,我们介绍了一种工程化的基于RNA的设备平台的开发,该平台可检测内源蛋白信号并对其起作用,将这些信号与基因的调控以及细胞功能联系起来。人类细胞中的内源基因。先前开发的RNA控制设备已在多种细胞类型中证明了可编程的配体响应遗传调控,我们尝试使此类顺式作用控制元件适应反式功能。我们将设备分为两条链,可在杂交后重新构建活性。使用体内模型系统优化了设备功能,我们发现设备序列不像以前报道的那样灵活。在验证了我们优化设计的体外活性之后,我们尝试使用其他元件来指导设备的稳定性,结构和定位,从而在人类细胞系中建立基因调控。我们平台的显着局限性阻止了内源性基因调控。我们接下来描述基于蛋白质反应的基于RNA的调控平台的发展。通过采用各种设计策略,我们展示了可响应人类细胞系中异源蛋白质的基因表达上调和下调的功能性设备。我们平台的活动超出了类似的小分子响应平台的活动。我们展示了我们的设备对细胞质和核定位蛋白有反应的能力,提供了对作用机理的洞察力,并将我们的平台与具有限制性更严格的配体定位要求的先前描述的设备区分开。最后,我们通过开发对内源性信号蛋白起反应的调控设备,证明了我们设备平台的多功能性。我们在此展示的基础工具相对于先前描述的基于RNA的基因调控平台具有独特的优势。这种基因编码技术可能会在开发更有效的诊断工具和靶向分子治疗策略中找到未来的应用。

著录项

  • 作者

    Vowles, James Vincent.;

  • 作者单位

    California Institute of Technology.;

  • 授予单位 California Institute of Technology.;
  • 学科 Chemistry.;Biomedical engineering.
  • 学位 Ph.D.
  • 年度 2014
  • 页码 164 p.
  • 总页数 164
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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