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Capped nucleic acid oligomers that inhibit cap-dependent transcription of the influenza virus endonuclease

机译:抑制流感病毒核酸内切酶帽依赖性转录的带帽核酸寡聚体

摘要

Novel capped oligonucleotides useful in treatment of influenza infection. A synthetically derived 67-nucleotide RNA substrate, containing a [.sup.32 P] labeled cap-1 structure was used to analyze parameters of influenza virus endonuclease activity. This substrate was specifically cleaved by the influenza virus polymerase to yield a single capped 11-nucleotide fragment capable of directly priming transcription. An analysis of systematic truncations of this RNA substrate in cleavage, elongation, and binding reactions demonstrated that the minimum chain length required for cleavage was one nucleotide past the cleavage site. In contrast, the minimum chain length required for priming activity was found to be 9 nucleotides, while a chain length of at least 4 nucleotides was required for efficient binding. Based on these chain length requirements, the present inventors show that a pool of capped oligonucleotides--too short to prime transcription but long enough to bind with high affinity to the viral polymerase--are potent inhibitors of cap-dependent in vitro transcription.
机译:用于治疗流感感染的新型带帽寡核苷酸。含有[32 P]标记的cap-1结构的合成衍生的67个核苷酸的RNA底物用于分析流感病毒核酸内切酶活性的参数。该底物被流感病毒聚合酶特异性切割,以产生能够直接引发转录的单个带帽的11个核苷酸片段。对该RNA底物在切割,延伸和结合反应中的系统截短的分析表明,切割所需的最小链长是切割位点后的一个核苷酸。相反,发现引发活性所需的最小链长为9个核苷酸,而有效结合需要至少4个核苷酸的链长。基于这些链长要求,本发明人表明,封端的寡核苷酸池太短以至于不能进行初次转录,但足够长以与病毒聚合酶高亲和力结合,是帽依赖性体外转录的有效抑制剂。

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