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A Trisbenzimidazole Phosphoramidite Building Block Enables High-Yielding Syntheses of RNA-Cleaving Oligonucleotide Conjugates

机译:Trisbenzimidazole亚磷酰胺的构建基块能够高产合成裂解RNA的寡核苷酸缀合物。

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摘要

The RNA cleaving catalyst tris(2-aminobenzimidazole) when attached to the 5’ terminus of oligonucleotides cuts complementary RNA strands in a highly site-specific manner. Conjugation was previously achieved by the acylation of an amino linker by an active ester of the catalyst. However, this procedure was low yielding and not reliable. Here, a phosphoramidite building block is described that can be coupled to oligonucleotides by manual solid phase synthesis in total yields around 85%. Based on this chemistry, we have now studied the impact of LNA (locked nucleic acids) nucleotides on the rates and the site-specificities of RNA cleaving conjugates. The highest reaction rates and the most precise cuts can be expected when the catalyst is attached to a strong 5’ closing base pair and when the oligonucleotide contains several LNA units that are equally distributed in the strand. However, when placed in the 5’ position, LNA building blocks tend to diminish the specificity of RNA cleavage.
机译:RNA裂解催化剂tris(2-氨基苯并咪唑)连接到寡核苷酸的5'末端时,会以高度位点特异性的方式切割互补的RNA链。先前通过催化剂的活性酯对氨基接头的酰化来实现偶联。但是,该方法收率低且不可靠。在此,描述了亚磷酰胺结构单元,其可以通过手动固相合成与寡核苷酸偶联,总产率约为85%。基于这种化学,我们现在研究了LNA(锁定核酸)核苷酸对RNA裂解偶联物的速率和位点特异性的影响。当催化剂连接到一个牢固的5'闭合碱基对上并且寡核苷酸包含几个均匀分布在链中的LNA单元时,可以预期到最高的反应速率和最精确的切割。但是,当置于5'位置时,LNA构建基块往往会降低RNA切割的特异性。

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