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脂质体与网状内皮系统的相互作用。II:小鼠腹腔巨噬细胞对脂质体的非特异性摄取和受体介导的摄取。

Interactions of liposomes with the reticuloendothelial system. II: Nonspecific and receptor-mediated uptake of liposomes by mouse peritoneal macrophages.

作者信息

Hsu M J, Juliano R L

出版信息

Biochim Biophys Acta. 1982 Jul 22;720(4):411-9. doi: 10.1016/0167-4889(82)90120-3.

Abstract

Liposomes are taken up as intact vesicles by mouse peritoneal macrophages in a process which is temperature sensitive and is affected by inhibitors of glycolytic metabolism and of microfilament activity. Macrophages take up negatively charge vesicles more readily than positively charged vesicles (2-fold) or neutral vesicles (4-fold). Macrophages take up similar amounts of multilamellar liposomes, reversed phase liposomes and small unilamellar liposomes in terms of lipids, however this corresponds to vastly different numbers of particles and amounts of trapped volume. Coating the liposomes with macromolecular ligands capable of interacting with macrophage surface receptors can markedly promote liposome uptake. Thus, formation of an IgG-antigen complex on the liposome surface results in a 10(2)-fold enhancement of liposome uptake, while coating the vesicles with fibronectin results in a 10-fold augmentation of uptake. Uptake via IgG-mediated and fibronectin-mediated processes seem to be independent since excess unlabelled, IgG-coated liposomes will inhibit the uptake of radioactively-labelled IgG-coated liposomes much more effectively than the uptake of radioactively-labelled fibronectin-coated liposomes. Cell-bound liposomes can readily be visualized on and inside of the macrophages using fluorescence microscopy techniques.

摘要

脂质体作为完整的囊泡被小鼠腹腔巨噬细胞摄取,该过程对温度敏感,并受糖酵解代谢抑制剂和微丝活性抑制剂的影响。巨噬细胞摄取带负电荷的囊泡比带正电荷的囊泡(2倍)或中性囊泡(4倍)更容易。就脂质而言,巨噬细胞摄取的多层脂质体、反相脂质体和小单层脂质体数量相似,然而这对应着截然不同的颗粒数量和包封体积。用能够与巨噬细胞表面受体相互作用的大分子配体包被脂质体可显著促进脂质体的摄取。因此,脂质体表面形成IgG - 抗原复合物会导致脂质体摄取增强100倍,而用纤连蛋白包被囊泡会使摄取增加10倍。通过IgG介导和纤连蛋白介导的摄取过程似乎是独立的,因为过量未标记的IgG包被脂质体比放射性标记的纤连蛋白包被脂质体更能有效抑制放射性标记的IgG包被脂质体的摄取。使用荧光显微镜技术可以很容易地在巨噬细胞表面和内部观察到细胞结合的脂质体。

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