首页> 外文期刊>Journal of Materials Chemistry, B. materials for biology and medicine >Identification of a potent ionizable lipid for efficient macrophage transfection and systemic anti-interleukin-1 beta siRNA delivery against acute liver failure
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Identification of a potent ionizable lipid for efficient macrophage transfection and systemic anti-interleukin-1 beta siRNA delivery against acute liver failure

机译:鉴定有效的可电离脂质,用于有效的巨噬细胞转染和全身抗白细胞介素-1βsiRNA递送免受急性肝衰竭的递送

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摘要

RNA interference (RNAi) therapy has great potential for treating inflammatory diseases. However, the development of potent carrier materials for delivering siRNA to macrophages is challenging. Herein, we design a set of ionizable lipid nanoparticles (LNPs) to screen and identify a potent carrier of siRNA for silencing an essential pro-inflammatory cytokine, interleukin-1 beta (IL-1 beta) in macrophages. The top performance LNP (114-LNP), containing ionizable lipid with spermine as an amine-head group, facilitated efficient siRNA internalization via multiple endocytosis pathways and achieved effective endosome escape in macrophages. The optimized LNP/siIL-1 beta achieved strong silencing of IL-1 beta in both activated Raw 264.7 cells and primary macrophages. Furthermore, systematic administration of 114-LNP/siIL-1 beta complexes could effectively inhibit IL-1 beta expression in an acute liver failure model and significantly attenuated hepatic inflammation and liver damage. These results suggest that the optimized ionizable lipid nanoparticle represents a promising platform for anti-inflammation therapies.
机译:RNA干扰(RNAi)疗法在治疗炎症性疾病方面具有巨大潜力。然而,开发向巨噬细胞输送siRNA的有效载体材料具有挑战性。在此,我们设计了一组可电离脂质纳米粒(LNPs)来筛选和鉴定siRNA的有效载体,以沉默巨噬细胞中的一种重要促炎症细胞因子白细胞介素-1β(IL-1β)。最高性能的LNP(114-LNP)含有可电离脂质,精胺作为胺头基团,通过多种内吞途径促进有效的siRNA内化,并在巨噬细胞中实现有效的内体逃逸。优化的LNP/siIL-1β在激活的Raw 264.7细胞和原代巨噬细胞中都实现了IL-1β的强烈沉默。此外,系统给药114-LNP/siIL-1β复合物可有效抑制急性肝衰竭模型中IL-1β的表达,并显著减轻肝脏炎症和肝损伤。这些结果表明,优化的可电离脂质纳米粒代表了一个有前途的抗炎治疗平台。

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