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Identification of metabolically stable 5 '- phosphate analogs that support single-stranded siRNA activity

机译:鉴定支持单链siRNA活性的代谢稳定的5'-磷酸类似物

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摘要

The ss-siRNA activity in vivo requires a metabolically stable 5 '-phosphate analog. In this report we used crystal structure of the 5 '-phosphate binding pocket of Ago-2 bound with guide strand to design and synthesize ss-siRNAs containing various 5 '-phosphate analogs. Our results indicate that the electronic and spatial orientation of the 5 '-phosphate analog was critical for ss-siRNA activity. Chemically modified ss-siRNA targeting human apoC III mRNA demonstrated good potency for inhibiting ApoC III mRNA and protein in transgenic mice. Moreover, ApoC III ss-siRNAs were able to reduce the triglyceride and LDL cholesterol in transgenic mice demonstrating pharmacological effect of ss-siRNA. Our study provides guidance to develop surrogate phosphate analog for ss-siRNA and demonstrates that ss-siRNA provides an alternative strategy for therapeutic gene silencing.
机译:体内的ss-siRNA活性需要代谢稳定的5'-磷酸类似物。在本报告中,我们使用了与引导链结合的Ago-2的5'-磷酸结合口袋的晶体结构来设计和合成包含各种5'-磷酸类似物的ss-siRNA。我们的结果表明5'-磷酸类似物的电子和空间取向对于ss-siRNA活性至关重要。化学修饰的靶向人apoC III mRNA的ss-siRNA在转基因小鼠中表现出了抑制ApoC III mRNA和蛋白质的良好能力。此外,ApoC III ss-siRNA能够降低转基因小鼠中的甘油三酸酯和LDL胆固醇,证明了ss-siRNA的药理作用。我们的研究为开发ss-siRNA的替代磷酸盐类似物提供指导,并证明ss-siRNA提供了治疗性基因沉默的替代策略。

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