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Small-sized stable lipid nanoparticle for the efficient delivery of siRNA to human immune cell lines

机译:小尺寸稳定的脂质纳米颗粒可有效地将siRNA传递至人类免疫细胞系

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摘要

Gene silencing by small interfering RNA (siRNA) is useful for analyzing the functions of human immune cells. However, the transfection of siRNA to human immune cells is difficult. Here, we used a multifunctional envelope-type nanodevice (MEND) containing YSK12-C4 (YSK12-MEND) to efficiently introduce siRNA to human immune cell lines, Jurkat, THP-1, KG-1 and NK92. The YSK12-MEND was transfected to human immune cell lines at a siRNA dose range of 1–30 nM, resulting that maximum gene silencing efficiencies at the mRNA level in Jurkat, THP-1, KG-1 and NK92 were 96%, 96%, 91% and 75%, respectively. The corresponding values for Lipofectamine RNAiMAX (RNAiMAX) were 37%, 56%, 43% and 19%, respectively. The process associated with cellular uptake played a role in effective gene silencing effect of the YSK12-MEND. The small size and high non-aggregability of the YSK12-MEND were advantageous for the cellular internalization of siRNA to immune cell lines. In the case of RNAiMAX, a drastic increase in particles size was observed in the medium used, which inhibited cellular uptake. The YSK12-MEND reported in herein appears to be appropriate for delivering siRNA to human immune cells, and the small particle size and non-aggregability are essential properties.
机译:小干扰RNA(siRNA)引起的基因沉默可用于分析人类免疫细胞的功能。然而,将siRNA转染至人免疫细胞是困难的。在这里,我们使用包含YSK12-C4(YSK12-MEND)的多功能包膜型纳米器件(MEND)将siRNA有效地引入人免疫细胞系Jurkat,THP-1,KG-1和NK92。 YSK12-MEND以1–30 nM的siRNA剂量转染至人类免疫细胞系,导致Jurkat,THP-1,KG-1和NK92在mRNA水平上的最大基因沉默效率分别为96%,96% ,分别为91%和75%。 Lipofectamine RNAiMAX(RNAiMAX)的相应值分别为37%,56%,43%和19%。与细胞摄取有关的过程在YSK12-MEND的有效基因沉默作用中起作用。 YSK12-MEND的小尺寸和高不可凝集性有助于siRNA在细胞内化成免疫细胞系。对于RNAiMAX,在使用的培养基中观察到粒径急剧增加,这抑制了细胞摄取。本文报道的YSK12-MEND似乎适合将siRNA递送至人免疫细胞,并且小粒径和不可凝集性是必不可少的性质。

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