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首页> 外文期刊>ACS Omega >Synthesis, Affinity for Complementary RNA and DNA, and Enzymatic Stability of Triazole-Linked Locked Nucleic Acids (t-LNAs)
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Synthesis, Affinity for Complementary RNA and DNA, and Enzymatic Stability of Triazole-Linked Locked Nucleic Acids (t-LNAs)

机译:三唑连接的锁定核酸(t-LNA)的合成,互补RNA和DNA的亲和力和酶稳定性。

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Dinucleoside phosphoramidites containing a triazole internucleotide linkage flanked by locked nucleic acid (LNA) were synthesized and incorporated into oligonucleotides (ONs). ONs bearing both LNA and triazole at multiple sites were obtained and their biophysical properties including enzymatic stability and binding affinity for RNA and DNA targets were studied. t-LNAs with four incorporations of a dinucleoside monomer having LNA on either side of the triazole linkage bind to their RNA target with significantly higher affinity and greater specificity than unmodified oligonucleotides, and are remarkably stable to nuclease degradation. A similar but reduced effect on enzymatic stability and binding affinity was noted for LNA only on the 3′-side of the triazole linkage. Thus, by combining unnatural triazole linkages and LNA in one unit (t-LNA), we produced a promising class of ONs with reduced anionic charge and potential for antisense applications.
机译:合成了侧接锁定核酸(LNA)的包含三唑核苷酸间键的二核苷亚磷酰胺,并将其掺入寡核苷酸(ON)中。获得了在多个位点同时具有LNA和三唑的ON,并且研究了它们的生物物理特性,包括酶稳定性和对RNA和DNA靶的结合亲和力。与三唑键的任一侧具有LNA的二核苷单体四次结合的t-LNA与未修饰的寡核苷酸相比具有显着更高的亲和力和更大的特异性结合至其RNA靶标,并且对核酸酶降解非常稳定。仅在三唑键的3'侧上观察到对LNA的酶稳定性和结合亲和力具有相似但降低的作用。因此,通过将非天然三唑键和LNA结合在一个单元(t-LNA)中,我们生产了一种前景广阔的ON,具有降低的阴离子电荷和用于反义应用的潜力。

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