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首页> 外文期刊>Nucleic Acids Research >Carrier-free cellular uptake and the gene-silencing activity of the lipophilic siRNAs is strongly affected by the length of the linker between siRNA and lipophilic group
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Carrier-free cellular uptake and the gene-silencing activity of the lipophilic siRNAs is strongly affected by the length of the linker between siRNA and lipophilic group

机译:siRNA和亲脂性基团之间的连接子的长度强烈影响无载体细胞吸收和亲脂性siRNA的基因沉默活性

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The conjugation of siRNA to molecules, which can be internalized into the cell via natural transport mechanisms, can result in the enhancement of siRNA cellular uptake. Herein, the carrier-free cellular uptake of nuclease-resistant anti-MDR1 siRNA equipped with lipophilic residues (cholesterol, lithocholic acid, oleyl alcohol and litocholic acid oleylamide) attached to the 5'-end of the sense strand via oligomethylene linker of various length was investigated. A convenient combination of H-phosphonate and phosphoramidite methods was developed for the synthesis of 5'-lipophilic conjugates of siRNAs. It was found that lipophilic siRNA are able to effectively penetrate into HEK293, HepG2 and KB-8-5 cancer cells when used in a micromolar concentration range. The efficiency of the uptake is dependent upon the type of lipophilic moiety, the length of the linker between the moiety and the siRNA and cell type. Among all the conjugates tested, the cholesterol-conjugated siRNAs with linkers containing from 6 to 10 carbon atoms demonstrate the optimal uptake and gene silencing properties: the shortening of the linker reduces the efficiency of the cellular uptake of siRNA conjugates, whereas the lengthening of the linker facilitates the uptake but retards the gene silencing effect and decreases the efficiency of the silencing.
机译:siRNA与分子的缀合可以通过自然转运机制内化到细胞中,可以导致siRNA细胞摄取的增强。在本文中,具有核酸亲和力的抗MDR1 siRNA的无载体细胞摄取,该脂质体通过各种长度的寡亚甲基接头连接到有义链的5'端,并具有亲脂残基(胆固醇,石蜡酸,油醇和石och酸油酰胺)被调查了。开发了一种方便的H-膦酸酯和亚磷酰胺方法的组合方法,用于合成siRNA的5'-亲脂性缀合物。已经发现,当以微摩尔浓度范围使用时,亲脂性siRNA能够有效渗透到HEK293,HepG2和KB-8-5癌细胞中。摄取的效率取决于亲脂性部分的类型,该部分与siRNA之间的接头长度以及细胞类型。在所有测试的缀合物中,具有6至10个碳原子的接头的胆固醇缀合siRNA表现出最佳的摄取和基因沉默特性:接头的缩短降低了siRNA缀合物的细胞摄取效率,而加长了接头促进摄取,但延迟基因沉默作用并降低沉默效率。

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