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具有不同聚乙二醇连接物的糖基化可逆加成-断裂链转移聚合物产生不同的短干扰 RNA 摄取、基因沉默和毒性特征。

Glycosylated Reversible Addition-Fragmentation Chain Transfer Polymers with Varying Polyethylene Glycol Linkers Produce Different Short Interfering RNA Uptake, Gene Silencing, and Toxicity Profiles.

机构信息

CSIRO Manufacturing , Private Bag 10, Clayton South, Victoria 3169, Australia.

CSIRO Health and Biosecurity , Port Arlington Rd, East Geelong, Victoria 3219, Australia.

出版信息

Biomacromolecules. 2017 Dec 11;18(12):4099-4112. doi: 10.1021/acs.biomac.7b01168. Epub 2017 Nov 9.

DOI:10.1021/acs.biomac.7b01168
PMID:29059528
Abstract

Achieving efficient and targeted delivery of short interfering (siRNA) is an important research challenge to overcome to render highly promising siRNA therapies clinically successful. Challenges exist in designing synthetic carriers for these RNAi constructs that provide protection against serum degradation, extended blood retention times, effective cellular uptake through a variety of uptake mechanisms, endosomal escape, and efficient cargo release. These challenges have resulted in a significant body of research and led to many important findings about the chemical composition and structural layout of the delivery vector for optimal gene silencing. The challenge of targeted delivery vectors remains, and strategies to take advantage of nature's self-selective cellular uptake mechanisms for specific organ cells, such as the liver, have enabled researchers to step closer to achieving this goal. In this work, we report the design, synthesis, and biological evaluation of a novel polymeric delivery vector incorporating galactose moieties to target hepatic cells through clathrin-mediated endocytosis at asialoglycoprotein receptors. An investigation into the density of carbohydrate functionality and its distance from the polymer backbone is conducted using reversible addition-fragmentation chain transfer polymerization and postpolymerization modification.

摘要

实现短干扰 (siRNA) 的高效和靶向递送是克服将极具前景的 siRNA 疗法转化为临床成功的重要研究挑战。在设计用于这些 RNAi 构建体的合成载体时存在挑战,这些载体提供了对血清降解、延长血液保留时间、通过多种摄取机制有效细胞摄取、内体逃逸和有效货物释放的保护。这些挑战产生了大量的研究,并导致了许多关于递送载体的化学组成和结构布局的重要发现,以实现最佳基因沉默。靶向递送载体的挑战仍然存在,并且利用自然的选择性细胞摄取机制将特定器官细胞(如肝脏)作为优势的策略,使研究人员更接近实现这一目标。在这项工作中,我们报告了一种新型聚合物递送载体的设计、合成和生物学评价,该载体整合了半乳糖部分,通过网格蛋白介导的内吞作用,通过去唾液酸糖蛋白受体靶向肝细胞。通过可逆加成-断裂链转移聚合和聚合后修饰,研究了碳水化合物功能密度及其与聚合物主链的距离。

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