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Receptors Endocytosis and Trafficking: the Biological Basis of Targeted Delivery of Antisense and siRNA Oligonucleotides

机译:受体内吞作用和贩运:靶向递送反义和siRNA寡核苷酸的生物学基础

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摘要

The problem of targeted delivery of antisense and siRNA oligonucleotides can be resolved into two distinct aspects. The first concerns devising ligand-oligonucleotide or ligand-carrier moieties that bind with high selectivity to receptors on the cell type of interest and that are efficiently internalized by endocytosis. The second concerns releasing oligonucleotides from pharmacologically inert endomembrane compartments so that they can access RNA in the cytosol or nucleus. In this review we will address both of these aspects. Thus we present information on three important receptor families, the integrins, the receptor tyrosine kinases, and the G protein-coupled receptors in terms of their suitability for targeted delivery of oligonucleotides. This includes discussion of receptor abundance, internalization and trafficking pathways, and the availability of suitable high affinity ligands. We also consider the process of oligonucleotide uptake and intracellular trafficking and discuss approaches to modulating these processes in a pharmacologically productive manner. Hopefully the basic information presented in this review will be of value to investigators involved in designing delivery approaches for oligonucleotides.
机译:靶向递送反义和siRNA寡核苷酸的问题可以解决为两个不同的方面。第一个问题涉及设计配体-寡核苷酸或配体-载体部分,该部分与目标细胞类型上的受体高选择性结合,并通过内吞作用有效地内在化。第二个问题涉及从药理惰性的内膜隔室释放寡核苷酸,以使它们可以进入细胞质或细胞核中的RNA。在这篇评论中,我们将解决这两个方面。因此,就它们对寡核苷酸的靶向递送的适用性而言,我们介绍了三个重要受体家族的信息,即整联蛋白,受体酪氨酸激酶和G蛋白偶联受体。这包括对受体丰度,内在化和运输途径的讨论,以及合适的高亲和力配体的可用性。我们还考虑了寡核苷酸摄取和细胞内运输的过程,并讨论了以药理学上有效的方式调节这些过程的方法。希望本文中介绍的基本信息对参与设计寡核苷酸递送方法的研究人员有价值。

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