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肺表面活性物质蛋白 C 和 D 在宿主防御鸟分枝杆菌中发挥不同的作用。

Pulmonary collectins play distinct roles in host defense against Mycobacterium avium.

机构信息

Department of Biochemistry, Sapporo Medical University School of Medicine, Sapporo 060-8556, Japan.

出版信息

J Immunol. 2011 Sep 1;187(5):2586-94. doi: 10.4049/jimmunol.1100024. Epub 2011 Aug 5.

DOI:10.4049/jimmunol.1100024
PMID:21821801
Abstract

Pulmonary collectins, surfactant protein A (SP-A) and surfactant protein D (SP-D), play important roles in the innate immunity of the lung. Mycobacterium avium is one of the well-known opportunistic pathogens that can replicate within macrophages. We examined the effects of pulmonary collectins in host defense against M. avium infection achieved via direct interaction between bacteria and collectins. Although both pulmonary collectins bound to M. avium in a Ca(2+)-dependent manner, these collectins revealed distinct ligand-binding specificity and biological activities. SP-A and SP-D bound to a methoxy group containing lipid and lipoarabinomannan, respectively. Binding of SP-D but not SP-A resulted in agglutination of M. avium. A chimeric protein with the carbohydrate recognition domain of SP-D, which chimera revealed a bouquet-like arrangement similar to SP-A, also agglutinated M. avium. The ligand specificity of the carbohydrate recognition domain of SP-D seems to be necessary for agglutination activity. The binding of SP-A strongly inhibited the growth of M. avium in culture media. Although pulmonary collectins did not increase membrane permeability of M. avium, they attenuated the metabolic rate of the bacteria. Observations under a scanning electron microscope revealed that SP-A almost completely covers bacterial surfaces, whereas SP-D binds to certain areas like scattered dots. These observations suggest that a distinct binding pattern of collectins correlates with the difference of their biological activities. Furthermore, the number of bacteria phagocytosed by macrophages was significantly increased in the presence of SP-D. These data indicate that pulmonary collectins play critical roles in host defense against M. avium.

摘要

肺表面活性物质相关蛋白 A(SP-A)和 D(SP-D)是肺固有免疫中的重要组成部分。鸟分枝杆菌是一种众所周知的机会性病原体,可以在巨噬细胞内复制。我们研究了肺表面活性物质相关蛋白在宿主防御中的作用,即通过细菌与表面活性物质相关蛋白的直接相互作用来实现。虽然两种肺表面活性物质相关蛋白都以 Ca(2+)依赖性方式与 M. avium 结合,但它们具有不同的配体结合特异性和生物学活性。SP-A 和 SP-D 分别与含有甲氧基的脂质和脂阿拉伯甘露聚糖结合。SP-D 结合但 SP-A 不结合导致 M. avium 凝集。具有 SP-D 糖识别域的嵌合蛋白也能凝集 M. avium,其呈现出类似于 SP-A 的花束样排列。SP-D 糖识别域的配体特异性似乎对于凝集活性是必需的。SP-A 强烈抑制 M. avium 在培养基中的生长。虽然肺表面活性物质相关蛋白不会增加 M. avium 的膜通透性,但它们会降低细菌的代谢率。扫描电子显微镜观察显示,SP-A 几乎完全覆盖细菌表面,而 SP-D 则像散在的点一样结合到某些区域。这些观察结果表明,表面活性物质相关蛋白的不同结合模式与它们的生物学活性差异相关。此外,在 SP-D 存在的情况下,巨噬细胞吞噬的细菌数量显著增加。这些数据表明肺表面活性物质相关蛋白在宿主防御 M. avium 中发挥关键作用。

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