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首页> 外文期刊>Biomacromolecules >siRNA-Loaded Polyion Complex Micelle Decorated with Charge-Conversional Polymer Tuned to Undergo Stepwise Response to Intra-Tumoral and Intra-Endosomal pHs for Exerting Enhanced RNAi Efficacy
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siRNA-Loaded Polyion Complex Micelle Decorated with Charge-Conversional Polymer Tuned to Undergo Stepwise Response to Intra-Tumoral and Intra-Endosomal pHs for Exerting Enhanced RNAi Efficacy

机译:带有电荷转换聚合物的siRNA负载聚离子复合物胶束,经过调整,可以逐步响应肿瘤内和内体pH值,从而发挥增强的RNAi功效

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摘要

Small interfering RNA (siRNA) needs an efficient delivery vehicle to reach the cytoplasm of target cells for successful RNA interference (RNA therapy. This study aimed to develop an siRNA-loaded polyion complex (PIC) micelle equipped with a smart polymeric shell featuring tumor targetability and endosome escapability for enhanced RNAi activity in cancer cells. To this end, an acidic pH-responsive polypeptide was designed to exert a stepwise change in its charged state from negative to modestly positive and highly positive in response to slightly acidic environment of tumor (pH similar to 6.7)and further lowered-pH condition of late endosomal compartments (pH similar to 5.0)respectively, for selective binding to cancer cell surface and subsequent endosome disruption. This polypeptide, termed PAsp(DET-CDM/DBCO), was synthesized by introducing acid-labile carboxydimethyl maleate (CDM) and dibenzylcydooctyne (DBCO) moieties into a polyaspartamide derivative bearing two-repeated aminoethylene side chains (PAsp(DET)). Then, PAsp(DET-CDM/DBCO) was installed on the surface of disulfide cross-linked PIC micelles prepared from cholesterol-modified siRNA (Chol-siRNA) and azide-poly(ethylene glycol)-b-poly[(3-mercaptopropylamidine)-L-lysine] (N-3-PEG-b-PLys(MPA)) through the copper-free click reaction. Successful PAsp(DET-CDM/DBCO) coverage of PIC micelles was confirmed by a significant decrease in zeta-potential as well as a narrowly distributed size of 40 urn. The PAsp(DET-CDM/DBCO)-installed micelles significantly improved the gene-silencing efficiency in cultured lung cancer cells, compared with nonmodified control micelles, especially after incubation at pH 6.7. This improved silencing activity was nicely correlated with the facilitated cellular uptake of siRNA payloads at the acidic pH and the efficient endosomal escape. These results demonstrate that the acidic pH-responsive polypeptide shell is a promising design strategy for tumor-targeted siRNA delivery.
机译:小型干扰RNA(siRNA)需要有效的转运载体才能到达靶细胞的细胞质,以成功进行RNA干扰(RNA治疗。这项研究的目的是开发装有siRNA的聚离子复合物(PIC)胶束,该胶束配备了具有肿瘤靶向性的智能聚合物外壳为此,设计了一种酸性pH响应多肽,以响应于肿瘤的弱酸性环境(pH),使电荷状态从负向逐步变为适度呈正和高度呈正性变化类似于6.7)并进一步降低晚期内体区室(pH类似于5.0)的pH条件,以选择性结合癌细胞表面和随后的内体破坏。该多肽被称为PAsp(DET-CDM / DBCO)将酸不稳定的马来酸羧二甲基酯(CDM)和二苄基环辛炔(DBCO)部分引入带有两个重复氨基乙基的聚天冬酰胺衍生物ne侧链(PAsp(DET))。然后,将PAsp(DET-CDM / DBCO)安装在由胆固醇修饰的siRNA(Chol-siRNA)和叠氮化物-聚(乙二醇)-b-聚[(3-巯基丙基am)制备的二硫键交联的PIC胶束表面上)-L-赖氨酸](N-3-PEG-b-PLys(MPA))通过无铜点击反应。 ζ电位显着降低以及40的窄分布尺寸证实了PIC胶束的成功的PAsp(DET-CDM / DBCO)覆盖。与未修饰的对照胶束相比,PAsp(DET-CDM / DBCO)胶束显着提高了培养的肺癌细胞的基因沉默效率,尤其是在pH 6.7下孵育后。这种提高的沉默活性与在酸性pH下促进细胞摄取siRNA有效负载和有效的内体逃逸密切相关。这些结果表明酸性pH响应多肽壳是肿瘤靶向的siRNA传递的有前途的设计策略。

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