Neutrophil-targeted, protease-activated pulmonary drug delivery blocks airway and systemic inflammation

中性粒细胞胞外陷阱 炎症 药物输送 中性粒细胞弹性蛋白酶 促炎细胞因子 免疫学 医学 脱颗粒 粘液纤毛清除率 药理学 化学 内科学 受体 有机化学
作者
Joscelyn C. Mejías,Osric Forrest,Camilla Margaroli,David Frey Rubio,Liliana Viera,Jindong Li,Xin Xu,Amit Gaggar,Rabindra Tirouvanziam,Krishnendu Roy
出处
期刊:JCI insight [American Society for Clinical Investigation]
卷期号:4 (23) 被引量:30
标识
DOI:10.1172/jci.insight.131468
摘要

Pulmonary drug delivery presents a unique opportunity to target lower airway inflammation, which is often characterized by the massive recruitment of neutrophils from blood. However, specific therapies are lacking modulation of airway neutrophil function, and difficult challenges must be overcome to achieve therapeutic efficacy against pulmonary inflammation, notably drug hydrophobicity, mucociliary and macrophage-dependent clearance, and high extracellular protease burden. Here, we present a multistage, aerodynamically favorable delivery platform that uses extracellular proteolysis to its advantage to deliver nanoparticle-embedded hydrophobic drugs to neutrophils within the lower airways. Our design consists of a self-regulated nanoparticle-in-microgel system, in which microgel activation is triggered by extracellular elastase (degranulated by inflammatory neutrophils), and nanoparticles are loaded with Nexinhib20, a potent neutrophil degranulation inhibitor. Successful in vivo delivery of Nexinhib20 to the airways and into neutrophils promoted resolution of the inflammatory response by dampening neutrophil recruitment and degranulation, proinflammatory cytokine production in both airway and systemic compartments, as well as the presence of neutrophil-derived pathological extracellular vesicles in the lung fluid. Our findings showcase a new platform that overcomes challenges in pulmonary drug delivery and allows customization to match the proteolytic footprint of given diseases.
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