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首页> 外文期刊>Biomaterials >High yield, scalable and remotely drug-loaded neutrophil-derived extracellular vesicles (EVs) for anti-inflammation therapy
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High yield, scalable and remotely drug-loaded neutrophil-derived extracellular vesicles (EVs) for anti-inflammation therapy

机译:用于抗炎疗法的高产,可伸缩和远程药物载体中性粒细胞衍生的细胞外囊泡(EVS)

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摘要

Extracellular vesicles (EVs) are nanoscale membrane-formed compartments naturally secreted from cells, which are intercellular mediators regulating physiology and pathogenesis, therefore they could be a novel therapeutic carrier for targeted delivery. However, the translation of EVs is hindered by the heterogeneous composition, low yield, inefficient drug loading and unlikely scalability. Here we report a strategy to generate EVs using nitrogen cavitation (NC-EVs) that instantly disrupts neutrophils to form nanosized membrane vesicles. NC-EVs are similar to naturally secreted EVs (NS-EVs), but contain less subcellular organelles and nuclear acids. The production of NC-EVs was increased by 16 folds and is easy to scale up for clinical use compared to NS-EVs. To examine the usefulness of NC-EVs as a drug delivery platform, piceatannol (an anti-inflammation drug) was remotely loaded in NC-EVs via the pH gradient. We found that piceatannol-loaded NC-EVs dramatically alleviated acute lung inflammation/injury and sepsis induced by lipopolysaccharide (LPS). Our studies reveal that nitrogen cavitation is a novel approach to efficiently generate EVs from any cell type and could be exploited for personalized nanomedicine. (C) 2017 Elsevier Ltd. All rights reserved.
机译:细胞外囊泡(EVS)是从细胞内自然分泌的纳米级膜形成隔室,其是调节生理和发病机制的细胞间介质,因此它们可以是用于靶向递送的新型治疗载体。然而,EVS的翻译被异质组合物,低产量,低效药物负载和不太可能的可扩展性阻碍。在这里,我们报告了使用氮气空化(NC-EV)产生EV的策略,该氮气静脉(NC-EV)瞬间破坏中性粒细胞以形成纳米化膜囊泡。 NC-EVS类似于天然分泌的EVS(NS-EV),但含有较少的亚细胞细胞器和核酸。与NS-EVS相比,NC-EVS的生产增加了16倍,易于扩大临床使用。为了检查NC-EVS作为药物递送平台的有用性,通过pH梯度将PICEATANNOL(抗炎药)远离NC-EV。我们发现Piceatannol加载的NC-EV显着缓解了脂多糖(LPS)诱导的急性肺炎/损伤和败血症。我们的研究表明,氮气空穴是一种新的方法,可以从任何细胞类型有效地产生EV,并且可以用于个性化纳米医生。 (c)2017 Elsevier Ltd.保留所有权利。

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