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Optimization of siRNA delivery to target sites: issues and future directions

机译:SiRNA交付的优化到目标网站:问题和未来方向

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ABSTRACT, Introduction: The discovery of RNA interference (RNAi) earned the 2006 Nobel Prize in Physiology or Medicine for its biological significance and potential for developing novel therapeutics. The small interfering RNA (siRNA) is the most promising tool for translating RNAi to clinical use. Efforts are ongoing to improve siRNA delivery through developing novel biomaterials and delivery strategies. Given time, it appears that siRNA drugs will eventually become a reality. Areas covered: The currently used approaches for siRNA delivery are discussed with a focus on siRNA therapeutics currently in clinical testing. A comparison of advantageous aspects of currently available platforms and the possibility of further optimization for increased efficiency and safety are presented. Future directions in siRNA delivery are also highlighted. Expert opinion: The recent success in the field of siRNA delivery is based mainly on developing new biomaterials with extraordinarily high activities. Notably, the introduction of ionizable lipids and novel targeting ligands represent two huge steps for realizing siRNA therapy. The currently available systems are largely directed to the liver and the new challenge is to extend their applicability for treating diseases of other organs. Active targeting to different organs is the most promising approach for developing new siRNA-based therapeutics.
机译:摘要,介绍:发现RNA干扰(RNAi)为其生理学或医学赢得了2006年的生理学或医学奖,以实现新的治疗方法的生物意义和潜力。小干扰RNA(siRNA)是将RNAi转化为临床使用的最有前途的工具。努力通过开发新的生物材料和交付策略来改善siRNA递送。给定时间,似乎siRNA药物最终将成为现实。所涵盖的区域:目前使用的siRNA交付方法是专注于目前临床检测中的siRNA治疗剂的讨论。介绍了当前可用平台的有利方面的比较以及进一步优化提高效率和安全性的可能性。 SiRNA交付中的未来方向也突出显示。专家意见:近期SiRNA交付领域的成功主要是在开发新的生物材料,具有非常高的活动。值得注意的是,引入可电离的脂质和新型靶向配体代表了实现siRNA治疗的两个巨大步骤。目前可用的系统主要针对肝脏,新的挑战是扩大其适用于治疗其他器官的疾病。对不同器官的活跃靶向是开发新的SiRNA治疗方法最有希望的方法。

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