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受生物启发的脂质体用于口服多粘菌素以对抗沙门氏菌引起的细胞内感染。

Bioinspired Liposomes for Oral Delivery of Colistin to Combat Intracellular Infections by Salmonella enterica.

机构信息

Helmholtz Institute for Pharmaceutical Research Saarland (HIPS), Helmholtz Center for Infection Research (HZI), Saarbrücken, 66123, Germany.

Department of Pharmacy, Saarland University, Saarbrücken, 66123, Germany.

出版信息

Adv Healthc Mater. 2019 Sep;8(17):e1900564. doi: 10.1002/adhm.201900564. Epub 2019 Jul 22.

DOI:10.1002/adhm.201900564
PMID:31328434
Abstract

Bacterial invasion into eukaryotic cells and the establishment of intracellular infection has proven to be an effective means of resisting antibiotic action, as anti-infective agents commonly exhibit a poor permeability across the host cell membrane. Encapsulation of anti-infectives into nanoscaled delivery systems, such as liposomes, is shown to result in an enhancement of intracellular delivery. The aim of the current work is, therefore, to formulate colistin, a poorly permeable anti-infective, into liposomes suitable for oral delivery, and to functionalize these carriers with a bacteria-derived invasive moiety to enhance their intracellular delivery. Different combinations of phospholipids and cholesterol are explored to optimize liposomal drug encapsulation and stability in biorelevant media. These liposomes are then surface-functionalized with extracellular adherence protein (Eap), derived from Staphylococcus aureus. Treatment of HEp-2 and Caco-2 cells infected with Salmonella enterica using colistin-containing, Eap-functionalized liposomes resulted in a significant reduction of intracellular bacteria, in comparison to treatment with nonfunctionalized liposomes as well as colistin alone. This indicates that such bio-invasive carriers are able to facilitate intracellular delivery of colistin, as necessary for intracellular anti-infective activity. The developed Eap-functionalized liposomes, therefore, present a promising strategy for improving the therapy of intracellular infections.

摘要

细菌侵入真核细胞并建立细胞内感染已被证明是一种有效的抗抗生素作用的手段,因为抗感染药物通常对宿主细胞膜的通透性较差。将抗感染药物封装到纳米级递药系统中,如脂质体,可导致细胞内递药的增强。因此,本研究的目的是将不易渗透的抗感染药物黏菌素制成适合口服递药的脂质体,并通过细菌衍生的侵袭性部分对这些载体进行功能化,以增强其细胞内递药。研究探索了不同的磷脂和胆固醇组合,以优化脂质体药物包封和在生物相关介质中的稳定性。然后,用来源于金黄色葡萄球菌的细胞外黏附蛋白 (Eap) 对这些脂质体进行表面功能化。用含有黏菌素的、Eap 功能化的脂质体处理感染沙门氏菌的 HEp-2 和 Caco-2 细胞,与用非功能化脂质体以及单独用黏菌素处理相比,细胞内细菌数量显著减少。这表明这种生物侵袭性载体能够促进黏菌素的细胞内递药,这是细胞内抗感染活性所必需的。因此,开发的 Eap 功能化脂质体为改善细胞内感染的治疗提供了一种有前途的策略。

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