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首页> 外文期刊>Infection and immunity >CD14 and CD11b mediate serum-independent binding to human monocytes of an acylpolygalactoside isolated from Klebsiella pneumoniae.
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CD14 and CD11b mediate serum-independent binding to human monocytes of an acylpolygalactoside isolated from Klebsiella pneumoniae.

机译:CD14和CD11b介导与肺炎克雷伯菌分离的酰基多聚半乳糖苷与人单核细胞的血清非依赖性结合。

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A water-soluble acylpolygalactosyl (APG) of 34 kDa was obtained from the Klebsiella pneumoniae membrane by alkaline hydrolysis and delipidation. APG comprises a poly(1,3)galactose chain, a core, and a lipid moiety made of a glucosamine disaccharide with two N-linked beta OH-myristates. The monocyte binding sites for APG were investigated by flow cytometry. Biotin-labelled APG (Biot-APG) bound to monocytes at 4 degrees C in the absence of serum, calcium, and magnesium. The binding was dose dependent, saturable, and displaced by unlabelled APG. Neither the polysaccharide chain present in APG-related molecules nor the PPi group or additional ester-linked myristates and palmitates were required for APG binding. The role of CD11b and CD14 was demonstrated by competitive inhibition with monoclonal antibodies and by the uptake of APG by these solubilized proteins. APG was rapidly internalized into monocytes at 37 degrees C while CD14 and CD11b/CD18 molecules were partially down-modulated. Lipopolysaccharides (LPS) from the same K. pneumoniae strain and from Escherichia coli and Salmonella minnesota partially competed for Biot-APG binding in the absence but not in the presence of serum. When altered by alkaline hydrolysis, those LPS became strong competitors for APG binding. It was concluded that alkaline hydrolysis of the K. pneumoniae membrane yielded molecules structurally related to LPS which bind to LPS membrane receptors in the absence of serum.
机译:通过碱性水解和脱脂从肺炎克雷伯氏菌膜获得34kDa的水溶性酰基聚半乳糖基(APG)。 APG包括一条聚(1,3)半乳糖链,一个核心和一个由氨基葡萄糖二糖与两个N-连接的β-羟基肉豆蔻酸酯组成的脂质部分。通过流式细胞术研究了APG的单核细胞结合位点。在没有血清,钙和镁的情况下,生物素标记的APG(Biot-APG)在4摄氏度下与单核细胞结合。结合是剂量依赖性的,可饱和的,并被未标记的APG取代。 APG结合不需要存在于APG相关分子中的多糖链,PPi基团或其他酯连接的肉豆蔻酸酯和棕榈酸酯。 CD11b和CD14的作用通过与单克隆抗体的竞争性抑制以及这些可溶蛋白对APG的吸收来证明。 APG在37摄氏度下迅速内化到单核细胞中,而CD14和CD11b / CD18分子被部分下调。来自相同的肺炎克雷伯菌菌株以及来自大肠杆菌和明尼苏达沙门氏菌的脂多糖(LPS)在不存在但不存在血清的情况下部分竞争Biot-APG结合。当被碱性水解改变时,那些LPS成为APG结合的强大竞争者。结论是,肺炎克雷伯菌膜的碱性水解产生与LPS结构相关的分子,该分子在没有血清的情况下与LPS膜受体结合。

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