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腺病毒-聚赖氨酸复合物将三链形成寡核苷酸有效递送至肿瘤细胞。

Efficient delivery of triplex forming oligonucleotides to tumor cells by adenovirus-polylysine complexes.

作者信息

Ebbinghaus S W, Vigneswaran N, Miller C R, Chee-Awai R A, Mayfield C A, Curiel D T, Miller D M

机构信息

University of Alabama at Birmingham, USA.

出版信息

Gene Ther. 1996 Apr;3(4):287-97.

PMID:8732160
Abstract

Oligonucleotides (ODNs) show great promise in their ability to specifically inhibit single gene expression but must cross the cell membrane, escape the endosomal vesicle, and possibly traverse the nuclear membrane to arrive at their intracellular target molecules. In an attempt to improve the delivery of phosphodiester triplex forming ODNs to malignant cells, we have constructed adenovirus-polylysine (AdpL)-ODN complexes designed to take advantage of the receptor mediated endocytosis of adenoviruses to transfer the ODNs to the cell nucleus. Treatment of several different types of tumor cells in culture by AdpL-ODN complex resulted in superior uptake and persistence of the ODNs compared to both free ODN and cationic lipid-ODN complexes. Nuclear uptake peaks at 4 h and intact ODN persists in the nucleus with a half-life of 12 h. ODN concentrations of 20-70 microM are achieved at 24 h in all monolayer cell lines evaluated to date. ODNs are detected in 50-100% of the total cell population by immunohistochemistry with apparent uptake into vesicles and nuclear localization. Luciferase expression of a co-delivered reporter plasmid suggests that these ODNs are free in the nucleus. AdpL-ODN complexes will provide a valuable tool for delivering unmodified ODNs to the nucleus of malignant cells.

摘要

寡核苷酸(ODNs)在特异性抑制单个基因表达方面显示出巨大潜力,但必须穿过细胞膜、逃离内体囊泡,并可能穿过核膜才能到达其细胞内靶分子。为了提高磷酸二酯三链形成ODNs向恶性细胞的递送效率,我们构建了腺病毒-聚赖氨酸(AdpL)-ODN复合物,旨在利用腺病毒的受体介导内吞作用将ODNs转移到细胞核。与游离ODN和阳离子脂质-ODN复合物相比,用AdpL-ODN复合物处理培养中的几种不同类型肿瘤细胞,导致ODNs的摄取和持久性更佳。核摄取在4小时达到峰值,完整的ODN在细胞核中持续存在,半衰期为12小时。在迄今为止评估的所有单层细胞系中,24小时时ODN浓度达到20-70微摩尔。通过免疫组织化学在50-100%的总细胞群体中检测到ODNs,明显摄取到囊泡中并定位于细胞核。共递送的报告质粒的荧光素酶表达表明这些ODNs在细胞核中是游离的。AdpL-ODN复合物将为将未修饰的ODNs递送至恶性细胞核提供一种有价值的工具。

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