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多功能金纳米粒子的设计用于体外和体内基因沉默。

Design of multifunctional gold nanoparticles for in vitro and in vivo gene silencing.

机构信息

Instituto de Nanociencia de Aragon, University of Zaragoza, C/Mariano Esquillor s/n Zaragoza, Spain.

出版信息

ACS Nano. 2012 Sep 25;6(9):8316-24. doi: 10.1021/nn3030223. Epub 2012 Aug 22.

Abstract

Over the past decade, the capability of double-stranded RNAs to interfere with gene expression has driven new therapeutic approaches. Since small interfering RNA (siRNAs, 21 base pair double-stranded RNA) was shown to be able to elicit RNA interference (RNAi), efforts were directed toward the development of efficient delivery systems to preserve siRNA bioactivity throughout the delivery route, from the administration site to the target cell. Here we provide evidence of RNAi triggering, specifically silencing c-myc protooncogene, via the synthesis of a library of novel multifunctional gold nanoparticles (AuNPs). The efficiency of the AuNPs is demonstrated using a hierarchical approach including three biological systems of increasing complexity: in vitro cultured human cells, in vivo invertebrate (freshwater polyp, Hydra ), and in vivo vertebrate (mouse) models. Our synthetic methodology involved fine-tuning of multiple structural and functional moieties. Selection of the most active functionalities was assisted step-by-step through functional testing that adopted this hierarchical strategy. Merging these chemical and biological approaches led to a safe, nonpathogenic, self-tracking, and universally valid nanocarrier that could be exploited for therapeutic RNAi.

摘要

在过去的十年中,双链 RNA 干扰基因表达的能力推动了新的治疗方法的发展。自从小干扰 RNA(siRNA,21 个碱基对的双链 RNA)被证明能够引发 RNA 干扰(RNAi)以来,人们一直致力于开发有效的递送系统,以在从给药部位到靶细胞的整个递送过程中保持 siRNA 的生物活性。在这里,我们通过合成一系列新型多功能金纳米粒子(AuNPs)提供了 RNAi 触发的证据,特别是通过合成来沉默 c-myc 原癌基因。我们使用包括三个越来越复杂的生物学系统的分层方法来证明 AuNPs 的效率:体外培养的人类细胞、体内无脊椎动物(淡水螅,Hydra)和体内脊椎动物(小鼠)模型。我们的合成方法涉及对多种结构和功能部分进行微调。通过采用这种分层策略的功能测试,逐步选择最有效的功能。将这些化学和生物学方法结合起来,得到了一种安全、无毒、自我追踪、普遍有效的纳米载体,可用于治疗性 RNAi。

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