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Oligonucleotide conjugates - Candidates for gene silencing therapeutics

机译:寡核苷酸共轭物-基因沉默疗法的候选人

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The potential therapeutic and diagnostic applications of oligonucleotides (ONs) have attracted great attention in recent years. The capability of ONs to selectively inhibit target genes through antisense and RNA interference mechanisms, without causing un-intended sideeffects has led them to be investigated for various biomedical applications, especially for the treatment of viral diseases and cancer. In recent years, many researchers have focused on enhancing the stability and target specificity of ONs by encapsulating/complexing them with polymers or lipid chains to formulate nanoparticlesanocom plexes/micelles. Also, chemical modification of nucleic acids has emerged as an alternative to impart stability to ONs against nucleases and other degrading enzymes and proteins found in blood. In addition to chemically modifying the nucleic acids directly, another strategy that has emerged, involves conjugating polymers/peptide/aptamers/antibodies/proteins, preferably to the sense strand (3'end) of siRNAs. Conjugation to the siRNA not only enhances the stability and targeting specificity of the siRNA, but also allows for the development of self-administering siRNA formulations, with a much smaller size than what is usually observed for nanoparticle (similar to 200 nm). This review concentrates mainly on approaches and studies involving ON-conjugates for biomedical applications. (C) 2016 Elsevier B.V. All rights reserved.
机译:近年来,寡核苷酸(ON)的潜在治疗和诊断应用引起了极大的关注。 ON通过反义和RNA干扰机制选择性抑制靶基因而不会引起意想不到的副作用的能力已导致它们被研究用于各种生物医学应用,尤其是用于治疗病毒性疾病和癌症。近年来,许多研究人员致力于通过将ONs与聚合物或脂质链封装/复合以配制纳米颗粒/纳米复合体/胶束,来增强ON的稳定性和靶标特异性。而且,已经出现了核酸的化学修饰作为赋予ONs以抵抗核酸酶和血液中发现的其他降解酶和蛋白质的稳定性的替代方案。除了直接化学修饰核酸之外,已经出现的另一种策略涉及将聚合物/肽/适体/抗体/蛋白质偶联,优选偶联至siRNA的有义链(3'末端)。与siRNA的缀合不仅增强了siRNA的稳定性和靶向特异性,而且允许开发自给药的siRNA制剂,其尺寸远小于通常观察到的纳米颗粒(类似于200 nm)的尺寸。这篇综述主要集中在涉及生物医学应用的ON-共轭物的方法和研究上。 (C)2016 Elsevier B.V.保留所有权利。

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