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Enhanced siRNA delivery using a combination of an Arginine-grafted bioreducible polymer, ultrasound, and microbubbles in cancer cells

机译:结合精氨酸嫁接的生物可还原聚合物,超声波和癌细胞中的微气泡增强siRNA传递

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摘要

RNAi-based gene therapy for cancer treatment has not shown significant clinical impact due to poor siRNA delivery to the target site. Here, we design a nonviral siRNA gene carrier using a combination of an arginine-grafted bioreducible polymer (ABP), microbubbles (MB), and ultrasound (US), for targeting vascular endothelial growth factor (VEGF) in a human ovarian cancer cell line. Newly designed MBs with a perfluorocrownether gas core show higher stability compared to controls. Further, MBs in combination with polyplexes show a significant higher loading capacity compared to naked siRNA. Lastly, only siRNA-ABP-MB (SAM) complexes in combination with US show significant VEGF knock down in A2780 human ovarian cancer cell line compared to naked siRNA when incubated for a short time after sonication treatment.
机译:由于不良的siRNA传递至靶位点,基于RNAi的基因治疗癌症尚未显示出明显的临床效果。在这里,我们设计了一种非病毒性siRNA基因载体,将精氨酸嫁接的生物可还原聚合物(ABP),微泡(MB)和超声(US)结合使用,以靶向人类卵巢癌细胞系中的血管内皮生长因子(VEGF) 。与对照相比,新设计的具有全氟冠醚气芯的MB表现出更高的稳定性。此外,与裸露的siRNA相比,MB与多链体结合显示出更高的负载能力。最后,在超声处理后短时间孵育时,与裸siRNA相比,只有siRNA-ABP-MB(SAM)复合物与US结合才能在A2780人卵巢癌细胞系中显示出显着的VEGF抑制作用。

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