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首页> 外文期刊>Nucleic Acids Research >CLEAVAGE OF TRNA WITH IMIDAZOLE AND SPERMINE IMIDAZOLE CONSTRUCTS - A NEW APPROACH FOR PROBING RNA STRUCTURE
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CLEAVAGE OF TRNA WITH IMIDAZOLE AND SPERMINE IMIDAZOLE CONSTRUCTS - A NEW APPROACH FOR PROBING RNA STRUCTURE

机译:含咪唑和精胺咪唑结构的TRNA切割-探究RNA结构的新方法。

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摘要

Hydrolysis of RNA in imidazole buffer and by spermine-imidazole conjugates has been investigated. The RNA models were yeast tRNA(Asp) and a transcript derived from the 3'-terminal sequence of tobacco mosaic virus RNA representing a minihelix capable of being enzymatically aminoacylated with histidine. Imidazole buffer and spermine-imidazole conjugates in the presence of free imidazole cleave phosphodiester bonds in the folded RNAs in a specific fashion. Imidazole buffer induces cleavages preferentially in single-stranded regions because nucleotides in these regions have more conformational freedom and can assume more easily the geometry needed for formation of the hydrolysis intermediate state. Spermine-imidazole constructs supplemented with free imidazole cleave tRNA(Asp) within single-stranded regions after pyrimidine residues with a marked preference for pyrimidine-A sequences. Hydrolysis patterns suggest a cleavage mechanism involving an attack by the imidazole residue of the electrostatically bound spermine-imidazole and by free imidazole at the most accessible single-stranded regions of the RNA. Cleavages in a viral RNA fragment recapitulating a tRNA-like domain were found in agreement with the model of this molecule that accounts for its functional properties, thus illustrating the potential of the imidazole-derived reagents as structural probes for solution mapping of RNAs. The cleavage reactions are simple to perform, provide information reflecting the state of the ribose-phosphate backbone of RNA and can be used for mapping single-and double-stranded regions in RNAs.
机译:已经研究了在咪唑缓冲液中和精胺-咪唑共轭物对RNA的水解作用。 RNA模型是酵母tRNA(Asp)和来自烟草花叶病毒RNA 3'端序列的转录本,代表能够被组氨酸酶促酰化的小螺旋。在游离咪唑存在下,咪唑缓冲液和精胺-咪唑共轭物以特定方式在折叠的RNA中裂解磷酸二酯键。咪唑缓冲液优先在单链区域诱导裂解,因为这些区域中的核苷酸具有更大的构象自由度,并且可以更轻松地呈现形成水解中间态所需的几何形状。精胺-咪唑构建体辅以游离咪唑后,在嘧啶残基后的单链区域内切割tRNA(Asp),并显着偏向嘧啶-A序列。水解模式表明了一种裂解机制,涉及到静电结合的精胺-咪唑的咪唑残基和RNA最易接近的单链区的游离咪唑的攻击。发现重现tRNA样结构域的病毒RNA片段中的裂解与该分子的说明其功能特性的模型一致,从而说明了咪唑衍生的试剂作为RNA溶液定位的结构探针的潜力。裂解反应易于进行,可提供反映RNA核糖磷酸骨架状态的信息,可用于定位RNA中的单链和双链区域。

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