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载有抗生素的岩藻糖基化脂质纳米载体有效地抑制了人髓样细胞中分枝杆菌的繁殖。

Fucosylated lipid nanocarriers loaded with antibiotics efficiently inhibit mycobacterial propagation in human myeloid cells.

机构信息

Institute for Experimental Infection Research, TWINCORE, Centre for Experimental and Clinical Infection Research, a joint venture between the Hannover Medical School and the Helmholtz Centre for Infection Research, Hannover, Germany.

Rodos Biotarget GmbH, Hannover, Germany.

出版信息

J Control Release. 2021 Jun 10;334:201-212. doi: 10.1016/j.jconrel.2021.04.012. Epub 2021 Apr 16.

Abstract

Antibiotic treatment of tuberculosis (TB) is complex, lengthy, and can be associated with various adverse effects. As a result, patient compliance often is poor, thus further enhancing the risk of selecting multi-drug resistant bacteria. Macrophage mannose receptor (MMR)-positive alveolar macrophages (AM) constitute a niche in which Mycobacterium tuberculosis replicates and survives. Therefore, we encapsulated levofloxacin in lipid nanocarriers functionalized with fucosyl residues that interact with the MMR. Indeed, such nanocarriers preferentially targeted MMR-positive myeloid cells, and in particular, AM. Intracellularly, fucosylated lipid nanocarriers favorably delivered their payload into endosomal compartments, where mycobacteria reside. In an in vitro setting using infected human primary macrophages as well as dendritic cells, the encapsulated antibiotic cleared the pathogen more efficiently than free levofloxacin. In conclusion, our results point towards carbohydrate-functionalized nanocarriers as a promising tool for improving TB treatment by targeted delivery of antibiotics.

摘要

结核病(TB)的抗生素治疗复杂、漫长,并可能伴有各种不良反应。因此,患者的依从性往往较差,从而进一步增加了选择耐多药细菌的风险。甘露糖受体(MMR)阳性肺泡巨噬细胞(AM)构成了分枝杆菌复制和存活的小生境。因此,我们将左氧氟沙星包封在脂质纳米载体中,这些纳米载体带有与 MMR 相互作用的岩藻糖残基。事实上,这种纳米载体优先靶向 MMR 阳性髓样细胞,特别是 AM。在使用感染的人原代巨噬细胞和树突状细胞的体外实验中,包封的抗生素比游离左氧氟沙星更有效地清除病原体。总之,我们的研究结果表明,糖基化纳米载体是一种很有前途的工具,可通过抗生素的靶向递送来改善结核病的治疗效果。

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