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Effective Delivery of PEGylated siRNA-Containing Lipoplexes to Extraperitoneal Tumours following Intraperitoneal Administration

机译:腹膜内给药后将含PEG化siRNA的脂质复合物有效地递送至腹膜外肿瘤

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摘要

Intraperitoneal (i.p.) administration of small interfering RNA (siRNA) has, to date, shown promise in treating tumours located within the peritoneal cavity. The ability of these siRNA molecules to reach extraperitoneal tumours following i.p. administration is, however, yet to be investigated. Here, we examined the impact of PEGylation on the biodistribution of i.p. administered nucleic acids-containing lipoplexes. We showed that in contrast to non-PEGylated liposomes, PEGylated liposomes can deliver siRNA efficiently to extraperitoneal tumours following i.p. administration, resulting in a 45% reduction in tumour size when the oncogene-targeted siRNA was used. This difference was likely contributed by the decreased uptake of PEGylated lipoplexes in the first-pass organs, and, in particular, we observed a 10-fold decrease in the macrophage uptake of these particles compared to non-PEGylated counterparts. Overall, our results indicated the potential of using PEGylated liposomes to deliver siRNA for the treatment of i.p. localized cancer with coexisting extraperitoneal metastasis.
机译:迄今为止,腹膜内(i.p.)施用小分子干扰RNA(siRNA)在治疗位于腹膜腔内的肿瘤方面显示出了希望。这些siRNA分子在腹腔镜手术后到达腹膜外肿瘤的能力。然而,行政管理尚待调查。在这里,我们研究了PEG化对i.p.的生物分布的影响。施用含核酸的脂质复合物。我们表明,与非聚乙二醇化脂质体相比,聚乙二醇化脂质体可在腹腔镜手术后有效地将siRNA传递至腹膜外肿瘤。当使用靶向癌基因的siRNA时,给药可减少肿瘤大小45%。这种差异可能是由于首过器官中PEG化脂质复合物的摄取减少所致,特别是,与非PEG化对应物相比,我们观察到这些颗粒的巨噬细胞摄取减少了10倍。总的来说,我们的结果表明使用聚乙二醇化脂质体递送siRNA进行i.p.治疗的潜力。伴有腹膜外转移的局部癌。

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