Interplay between mucus mobility and alveolar macrophage targeting of surface-modified liposomes

脂质体 乙二醇 体内 透明质酸 化学 粘液 PEG比率 体外 生物物理学 粘蛋白 细胞生物学 生物化学 医学 生物 有机化学 生态学 生物技术 财务 解剖 经济
作者
Kamila Bohne Japiassu,François Fay,Alessandro Marengo,Younès Louaguenouni,Catherine Cailleau,Stéphanie Denis,David Chapron,Nicolas Tsapis,Thaís Leite Nascimento,Eliana Martins Lima,Elias Fattal
出处
期刊:Journal of Controlled Release [Elsevier BV]
卷期号:352: 15-24 被引量:6
标识
DOI:10.1016/j.jconrel.2022.10.006
摘要

Alveolar macrophages play a crucial role in the initiation and resolution of the immune response in the lungs. Pro-inflammatory M1 alveolar macrophages are an interesting target for treating inflammatory and infectious pulmonary diseases. One commune targeting strategy is to use nanoparticles conjugated with hyaluronic acid, which interact with CD44 overexpressed on the membrane of those cells. Unfortunately, this coating strategy may be countered by the presence on the surface of the nanoparticles of a poly(ethylene glycol) corona employed to improve nanoparticles' diffusion in the lung mucus. This study aims to measure this phenomenon by comparing the behavior in a murine lung inflammation model of three liposomal platforms designed to represent different poly(ethylene glycol) and hyaluronic acid densities (Liposome-PEG, Liposome-PEG-HA and Liposome-HA). In this work, the liposomes were obtained by a one-step ethanol injection method. Their interaction with mucin and targeting ability toward pro-inflammatory macrophages were then investigated in vitro and in vivo in a LPS model of lung inflammation. In vitro, poly(ethylene glycol) free HA-liposomes display a superior targeting efficiency toward M1 macrophages, while the addition of poly(ethylene glycol) induces better mucus mobility. Interestingly in vivo studies revealed that the three liposomes showed distinct cell specificity with alveolar macrophages demonstrating an avidity for poly(ethylene glycol) free HA-liposomes, while neutrophils favored PEGylated liposomes exempt of HA. Those results could be explained by the presence of two forces exercising a balance between mucus penetration and receptor targeting. This study corroborates the importance of considering the site of action and the targeted cells when designing nanoparticles to treat lung diseases.
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