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RNA-Based Drugs: From RNA Interference to Short Interfering RNAs

机译:基于RNA的药物:从RNA干扰到短干扰RNA

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摘要

RNA interference consists of a sequence specific post-transcriptional gene silencing phenomenon triggered by a double strand RNA molecule homologous to the silenced gene. The dsRNA is cleaved by DICER enzyme in small dsRNA pieces, named short interfering RNAs (siRNAs). These fragments are thereafter associated to RISC complex where the cleavage of target RNA occurs. The observation that siRNAs can trigger the RNA interference mechanism in mammalian cells represents a fundamental discovery that discloses new horizons in genetic researches in that theoretically each gene can be silenced. The relative simplicity by which active short interfering RNAs can be designed and synthesized explains their widespread use in basic and applied researches, even if appropriate controls that exclude off-target effects are strictly required. The findings that siRNAs are active even when expressed in viral vectors open the possibility that they can be very soon used for gene therapy of several human diseases.
机译:RNA干扰由与沉默基因同源的双链RNA分子触发的序列特异性转录后基因沉默现象组成。 dsRNA被DICER酶切割成小的dsRNA小片段,称为短干扰RNA(siRNA)。这些片段随后与发生靶RNA切割的RISC复合物相关。 siRNA可以触发哺乳动物细胞中RNA干扰机制的发现代表了一项基本发现,该发现揭示了遗传研究的新领域,即理论上每个基因都可以沉默。可以设计和合成活性短干扰RNA的相对简单性,说明了它们在基础研究和应用研究中的广泛应用,即使严格要求排除靶外效应的适当对照也是如此。 siRNA即使在病毒载体中表达时仍具有活性的发现打开了将其很快用于多种人类疾病的基因治疗的可能性。

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