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首页> 外文期刊>RSC Advances >Antisense oligonucleotide modified with serinol nucleic acid (SNA) induces exon skipping in mdx myotubes
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Antisense oligonucleotide modified with serinol nucleic acid (SNA) induces exon skipping in mdx myotubes

机译:用丝氨醇核酸 (SNA) 修饰的反义寡核苷酸诱导 mdx 肌管中的外显子跳跃

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Serinol nucleic acid (SNA) is a novel nucleic acid analogue that can form highly stable heteroduplexes with complementary DNA and RNA sequences. Structurally, SNA is a close mimic to peptide nucleic acid (PNA) which is widely used in diagnostic and therapeutic applications. SNA chemistry is relatively new, and so far the scope of SNA has only been explored in improving the efficacy of small interfering RNA and for developing a highly sensitive molecular beacon for diagnostic applications. In this study, we investigated the potential of SNA-modified antisense oligonucleotide (AO) in parallel to PNA-oligo for splicemodulation in an in vitro cellular model of Duchenne muscular dystrophy (DMD). We synthesized a 20mer SNA and PNA antisense oligonucleotide (AO) designed to induce exon-23 skipping in the mouse dystrophin gene transcript. Our results demonstrated that the SNA AO induced exon-23 skipping at all tested concentrations, whereas the corresponding PNA AO failed to induce any exon-23 skipping upon 24 hours of transfection using Lipofectin transfection reagent. Our results further expands the potential of SNA oligonucleotides in therapeutic applications.
机译:丝氨醇核酸(SNA)是一种新型核酸类似物,可以形成具有互补DNA和RNA序列的高度稳定的异源双链体。在结构上,SNA与肽核酸(PNA)非常相似,广泛用于诊断和治疗应用。SNA化学相对较新,到目前为止,SNA的范围仅在提高小干扰RNA的功效和开发用于诊断应用的高灵敏度分子信标方面进行了探索。在这项研究中,我们研究了 SNA 修饰的反义寡核苷酸 (AO) 与 PNA-寡核苷酸平行在杜氏肌营养不良症 (DMD) 的体外细胞模型中进行剪接调节的潜力。我们合成了 20mer SNA 和 PNA 反义寡核苷酸 (AO),旨在诱导小鼠抗肌萎缩蛋白基因转录本中的外显子 23 跳跃。我们的结果表明,SNA AO 在所有测试浓度下诱导外显子 23 跳跃,而相应的 PNA AO 在使用 Lipofectin 转染试剂转染 24 小时后未能诱导任何外显子 23 跳跃。我们的研究结果进一步扩大了SNA寡核苷酸在治疗应用中的潜力。

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