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三链螺旋的形成及用于基因表达序列特异性调控的反基因策略。

Triple helix formation and the antigene strategy for sequence-specific control of gene expression.

作者信息

Praseuth D, Guieysse A L, Hélène C

机构信息

Laboratoire de Biophysique, INSERM U201, CNRS UMR 8646, Muséum National d'Histoire Naturelle, Paris, France.

出版信息

Biochim Biophys Acta. 1999 Dec 10;1489(1):181-206. doi: 10.1016/s0167-4781(99)00149-9.

Abstract

Specific gene expression involves the binding of natural ligands to the DNA base pairs. Among the compounds rationally designed for artificial regulation of gene expression, oligonucleotides can bind with a high specificity of recognition to the major groove of double helical DNA by forming Hoogsteen type bonds with purine bases of the Watson-Crick base pairs, resulting in triple helix formation. Although the potential target sequences were originally restricted to polypurine-polypyrimidine sequences, considerable efforts were devoted to the extension of the repertoire by rational conception of appropriate derivatives. Efficient tools based on triple helices were developed for various biochemical applications such as the development of highly specific artificial nucleases. The antigene strategy remains one of the most fascinating fields of triplex application to selectively control gene expression. Targeting of genomic sequences is now proved to be a valuable concept on a still limited number of studies; local mutagenesis is in this respect an interesting application of triplex-forming oligonucleotides on cell cultures. Oligonucleotide penetration and compartmentalization in cells, stability to intracellular nucleases, accessibility of the target sequences in the chromatin context, the residence time on the specific target are all limiting steps that require further optimization. The existence and the role of three-stranded DNA in vivo, its interaction with intracellular proteins is worth investigating, especially relative to the regulation of gene transcription, recombination and repair processes.

摘要

特定基因表达涉及天然配体与DNA碱基对的结合。在为人工调控基因表达而合理设计的化合物中,寡核苷酸可通过与沃森-克里克碱基对的嘌呤碱基形成Hoogsteen型键,以高特异性识别结合到双螺旋DNA的大沟中,从而形成三链螺旋。尽管潜在的靶序列最初局限于聚嘌呤-聚嘧啶序列,但人们通过合理设计合适的衍生物,致力于扩大其范围。基于三链螺旋开发了高效工具,用于各种生化应用,如开发高特异性人工核酸酶。反基因策略仍然是三链体应用于选择性控制基因表达最具吸引力的领域之一。目前在数量仍然有限的研究中,基因组序列靶向已被证明是一个有价值的概念;在这方面,局部诱变是三链体形成寡核苷酸在细胞培养中的一个有趣应用。寡核苷酸在细胞中的渗透和区室化、对细胞内核酶的稳定性、染色质环境中靶序列的可及性、在特定靶标上的停留时间,都是需要进一步优化的限制步骤。三链DNA在体内的存在及其作用、它与细胞内蛋白质的相互作用值得研究,特别是相对于基因转录、重组和修复过程的调控而言。

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