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首页> 外文期刊>Nanoscale >The role of apolipoprotein- and vitronectin-enriched protein corona on lipid nanoparticles for in vivo targeted delivery and transfection of oligonucleotides in murine tumor models
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The role of apolipoprotein- and vitronectin-enriched protein corona on lipid nanoparticles for in vivo targeted delivery and transfection of oligonucleotides in murine tumor models

机译:载脂蛋白的作用,在脂质vitronectin-enriched蛋白质电晕体内的靶向纳米颗粒转染小鼠肿瘤的寡核苷酸模型

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摘要

The application of lipid-based nanoparticle (LNP) delivery systems remains a popular strategy for the systemic delivery of gene therapies to specific disease targets, including solid tumors. It is now well acknowledged that upon systemic administration, biomolecules from blood will adsorb onto nanoparticles' surfaces, forming a "protein corona", affording nanoparticles a "biological identity" on top of their "synthetic identity". Detailed analysis of nanoparticle protein corona is gradually revealing the "missing link" between nanoparticle chemical properties and the biological identity. Nevertheless, the discovery of nanoparticle protein corona's impact on tumor delivery is limited. In this study, we demonstrate that protein corona can be manipulated by formulation composition and particle surface charge changes, and a single lipid switch could switch the nanoparticle protein corona profile. The protein corona composition differences had a profound impact on cell transfection, in vivo biodistribution as well as tumor-specific delivery efficiency. Nanoparticles with apolipoprotein-rich corona showed better delivery to hepatocellular carcinoma (HepG2) as compared to those with vitronectin-rich corona. In addition, we found that, the PEG conjugated lipid chain length and PEG amount in LNPs were key factors to consider in successful RNA interference therapy for solid tumors.
机译:应用lipid-based纳米颗粒(LNP)运载系统仍然是一个受欢迎的策略基因疗法的系统交付特定疾病的目标,包括实体肿瘤。现在也承认,在系统性管理、生物分子从血液吸附在纳米颗粒的表面,形成一个“蛋白质冕”,提供纳米颗粒“生物身份”之上的“合成身份”。蛋白质电晕逐渐暴露纳米化学之间的“缺失的环节”属性和生物标识。然而,纳米粒子的发现蛋白质电晕对肿瘤的影响交付有限的。蛋白质日冕可以被制定成分和颗粒表面电荷变化,和一个脂质开关可以切换纳米蛋白质电晕概要文件。电晕有着深远的成分差异对细胞转染的影响,体内biodistribution以及肿瘤特异性交付效率。apolipoprotein-rich电晕显示更好的交付肝细胞癌(HepG2)相比那些vitronectin-rich日冕。此外,我们发现,共轭油脂挂钩链的长度和数量挂钩的现况是关键考虑因素在成功的RNA干预治疗实体肿瘤。

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