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Interplay of polyethyleneimine molecular weight and oligonucleotide backbone chemistry in the dynamics of antisense activity

机译:聚乙烯亚胺分子量与寡核苷酸主链化学在反义活性动力学中的相互作用

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摘要

The widespread utilization of gene silencing techniques, such as antisense, is impeded by the poor cellular delivery of oligonucleotides (ONs). Rational design of carriers for enhanced ON delivery demands a better understanding of the role of the vector on the extent and time course of antisense effects. The aim of this study is to understand the effects of polymer molecular weight (MW) and ON backbone chemistry on antisense activity. Complexes were prepared between branched polyethyleneimine (PEI) of various MWs and ONs of phosphodiester and phosphorothioate chemistries. We measured their physico-chemical properties and evaluated their ability to deliver ONs to cells, leading to an antisense response. Our key finding is that the antisense activity is not determined solely by PEI MW or by ON chemistry, but rather by the interplay of both factors. While the extent of target mRNA down-regulation was determined primarily by the polymer MW, dynamics were determined principally by the ON chemistry. Of particular importance is the strength of interactions between the carrier and the ON, which determines the rate at which the ONs are delivered intracellularly. We also present a mathematical model of the antisense process to highlight the importance of ON delivery to antisense down-regulation.
机译:基因沉默技术(例如反义)的广泛使用受到寡核苷酸(ON)的细胞递送不良的阻碍。为了增强ON传递而对载体进行合理设计,需要更好地理解载体在反义作用的程度和时间过程中的作用。这项研究的目的是了解聚合物分子量(MW)和骨架化学对反义活性的影响。在各种分子量的支化聚乙烯亚胺(PEI)与磷酸二酯和硫代磷酸酯化学试剂的ON之间制备了配合物。我们测量了它们的理化性质,并评估了它们将ONs传递至细胞的能力,从而导致了反义反应。我们的主要发现是,反义活性并非仅由PEI MW或ON化学决定,而是由两个因素的相互作用决定。虽然目标mRNA下调的程度主要由聚合物MW决定,但动力学主要由ON化学决定。特别重要的是载体与ON之间相互作用的强度,它决定了ON在细胞内传递的速率。我们还提出了反义过程的数学模型,以突出ON传递对反义下调的重要性。

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