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层状双氢氧化物纳米粒子的粒径减小可提高 siRNA 的递送效率。

Reduction in the size of layered double hydroxide nanoparticles enhances the efficiency of siRNA delivery.

机构信息

Queensland Brain Institute, The University of Queensland, Queensland 4072, Australia.

出版信息

J Colloid Interface Sci. 2013 Jan 15;390(1):275-81. doi: 10.1016/j.jcis.2012.09.033. Epub 2012 Sep 26.

Abstract

Small interfering RNAs (siRNAs) are a potentially powerful new class of pharmaceutical drugs for many disease. However, the delivery of unprotected siRNAs is ineffective due to their susceptibility to degradation by ubiquitous nucleases under physiological conditions. Layered double hydroxide nanoparticles (LDHs) have been found to be efficient carriers of anionic drugs and nucleic acids. Our previous research has shown that LDHs (with the Z-average particle size of approximately 110 nm) can mediate siRNA delivery in mammalian cells, resulting in gene silencing. However, short double-stranded nucleic acids are mostly adsorbed onto the external surface and not well protected by LDHs. In order to enhance the intercalation of siRNA into the LDH interlayer and the efficiency of subsequent siRNA delivery, we prepared smaller LDHs (with the Z-average particle size of approximately 45 nm) with an engineered non-aqueous method. We demonstrate here that dsDNA/siRNA is more effectively intercalated into these small LDH nanoparticles, more dsDNA/siRNA is transfected into HEK 293T cells, and more efficient silencing of the target gene is achieved using smaller LDHs. Thus, smaller LDH particles have greater potential as a delivery system for the application of RNA interference.

摘要

小干扰 RNA(siRNA)是一类有潜力的新型药物,可用于多种疾病的治疗。然而,由于其在生理条件下容易被普遍存在的核酸酶降解,未保护的 siRNA 的递送效果不佳。层状双氢氧化物纳米粒子(LDHs)已被发现是阴离子药物和核酸的有效载体。我们之前的研究表明,LDHs(平均粒径约为 110nm)可以介导哺乳动物细胞中的 siRNA 递送,从而实现基因沉默。然而,短双链核酸大多被吸附在外部表面,不能被 LDHs 很好地保护。为了增强 siRNA 插入 LDH 夹层的能力并提高随后的 siRNA 递送效率,我们采用工程化的非水方法制备了粒径更小(平均粒径约为 45nm)的 LDHs。我们在这里证明,dsDNA/siRNA 更有效地插入这些小的 LDH 纳米颗粒中,更多的 dsDNA/siRNA 被转染到 HEK 293T 细胞中,并且使用较小的 LDHs 可以更有效地实现靶基因的沉默。因此,较小的 LDH 颗粒作为 RNA 干扰应用的递送系统具有更大的潜力。

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