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Triplex-forming oligonucleotides - sequence-specific DNA ligands as tools for gene inhibition and for modulation of DNA-associated functions.

机译:形成三链体的寡核苷酸-特定于序列的DNA配体作为抑制基因和调节DNA相关功能的工具。

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摘要

The down regulation of gene expression is a promising strategy for molecular medicine and experimental biology. Molecules that bind to the DNA double helix may interfere with gene expression and, in addition to potential therapeutic applications, can be helpful for the investigation of DNA processing, chromatin package, or associated biological processes. Triplex-forming oligonucleotides (TFOs) bind to specific sequences in the DNA double helix via hydrogen bonding interactions. TFOs have been shown to down-regulate gene expression, to induce targeted genomic DNA modifications, to stimulate DNA recombination, and to modulate chromatin organization. Additionally, they may be used as carriers to position DNA-modifying agents to selected sequences. TFO-mediated effects have been mostly described in cell culture, but one study reported TFO activity in a mouse model. Critical issues regarding TFO-based technologies are the development of new oligonucleotide analogues with improved binding affinity, better target selectivity, and sufficient stability in the intracellular environment. A prerequisite for the development of such DNA-binding molecules is the availability of appropriate methods to assess their binding properties quantitatively at the desired target sequence in the genome. This review focuses on recent results regarding gene-inhibitory effects of TFOs in cell culture and methods to evaluate TFO-binding to the desired target sequence in the context of the human genome.
机译:基因表达的下调是分子医学和实验生物学的有前途的策略。与DNA双螺旋结合的分子可能会干扰基因表达,并且除了潜在的治疗应用外,还有助于研究DNA加工,染色质包装或相关的生物学过程。通过氢键相互作用,形成三链体的寡核苷酸(TFO)与DNA双螺旋中的特定序列结合。 TFO已显示出下调基因表达,诱导靶向基因组DNA修饰,刺激DNA重组和调节染色质组织。另外,它们可以用作将DNA修饰剂定位于所选序列的载体。 TFO介导的作用主要描述于细胞培养中,但一项研究报道了TFO在小鼠模型中的活性。关于基于TFO的技术的关键问题是开发具有改善的结合亲和力,更好的靶标选择性以及在细胞内环境中足够的稳定性的新型寡核苷酸类似物。发展这种DNA结合分子的先决条件是可获得合适的方法以定量地评估基因组中所需靶序列的结合特性。这篇综述的重点是有关TFO在细胞培养中的基因抑制作用的最新结果,以及在人类基因组背景下评估TFO与所需靶序列结合的方法。

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