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Locked nucleic acid (LNA) mediated improvements in siRNA stability and functionality

机译:锁定核酸(LNA)介导的siRNA稳定性和功能性改善

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摘要

Therapeutic application of the recently discovered small interfering RNA (siRNA) gene silencing phenomenon will be dependent on improvements in molecule bio-stability, specificity and delivery. To address these issues, we have systematically modified siRNA with the synthetic RNA-like high affinity nucleotide analogue, Locked Nucleic Acid (LNA). Here, we show that incorporation of LNA substantially enhances serum half-life of siRNA's, which is a key requirement for therapeutic use. Moreover, we provide evidence that LNA is compatible with the intracellular siRNA machinery and can be used to reduce undesired, sequence-related off-target effects. LNA-modified siRNAs targeting the emerging disease SARS, show improved efficiency over unmodified siRNA on certain RNA motifs. The results from this study emphasize LNA's promise in converting siRNA from a functional genomics technology to a therapeutic platform.
机译:最近发现的小干扰RNA(siRNA)基因沉默现象的治疗应用将取决于分子生物稳定性,特异性和递送的改善。为了解决这些问题,我们已经使用合成的类RNA高亲和力核苷酸类似物锁核酸(LNA)系统修饰了siRNA。在这里,我们表明掺入LNA可以大大提高siRNA的血清半衰期,这是治疗用途的关键要求。此外,我们提供的证据表明LNA与细胞内siRNA机制兼容,可用于减少不需要的,与序列相关的脱靶效应。靶向新兴疾病SARS的LNA修饰siRNA在某些RNA图案上比未修饰siRNA表现出更高的效率。这项研究的结果强调了LNA在将siRNA从功能基因组学技术转化为治疗平台方面的承诺。

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