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Performance of Pyridylthiourea‐Polyethylenimine Polyplex for siRNA‐Mediated Liver Cancer Therapy in Cell Monolayer, Spheroid, and Tumor Xenograft Models

机译:在细胞单层,球体和肿瘤异种移植模型中,吡啶基硫脲-聚乙烯亚胺复合物在siRNA介导的肝癌治疗中的性能

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Medical application of siRNAs relies on methods for delivering nucleic acids into the cytosol. Synthetic carriers, which assemble with nucleic acids into delivery systems, show promises for cancer therapy but efficiency remains to be improved. In here, the effectiveness of pyridylthiourea‐polyethylenimine (πPEI), a siRNA carrier that favors both polyplex disassembly and endosome rupture upon sensing the acidic endosomal environment, in 3 experimental models of hepatocellular cancer is tested. The πPEI‐assisted delivery of a siRNA targeting the polo‐like kinase 1 into Huh‐7 monolayer produces a 90% cell death via a demonstrated RNA interference mechanism. Incubation of polyplex with Huh‐7 spheroids leads to siRNA delivery into the superficial first cell layer and a 60% reduction in spheroid growth compared to untreated controls. Administration of polyplexes into mice bearing subcutaneous implanted Huh‐7Luc tumors results in a reduced tumor progression, similar to the one observed in the spheroid model. Altogether, these results support the in vivo use of synthetic and dedicated polymers for increasing siRNA‐mediated gene knockdown, and their clinical promise in cancer therapeutics.
机译:siRNA的医学应用依赖于将核酸输送到细胞质中的方法。与核酸组装成递送系统的合成载体显示出有望用于癌症治疗,但效率仍有待提高。在本文中,在3种肝细胞癌实验模型中,测试了吡啶基硫脲-聚乙烯亚胺(πPEI)(一种在感测到酸性内体环境后同时支持多链体分解和内体破裂的siRNA载体)的有效性。 πPEI辅助将靶向polo样激酶1的siRNA传递到Huh-7单层中,通过证实的RNA干扰机制可产生90%的细胞死亡。与未经处理的对照组相比,将复合物与Huh-7球体一起孵育可导致siRNA进入表层第一细胞层,并使球体生长降低60%。向患有皮下植入的Huh-7Luc肿瘤的小鼠施用多聚体可降低肿瘤进展,类似于在椭球模型中观察到的情况。总而言之,这些结果支持在体内使用合成和专用聚合物来增加siRNA介导的基因敲低,以及它们在癌症治疗中的临床前景。

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