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Purification and characterization of novel hemagglutinins from Vibrio mimicus: a 39-kilodalton major outer membrane protein and lipopolysaccharide.

机译:来自拟态弧菌的新型血凝素的纯化和鉴定:39千达尔顿的主要外膜蛋白和脂多糖。

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Two hemagglutinins (HAs) mediating the agglutinability to rabbit erythrocytes were isolated from 32-h culture supernatant of enterotoxigenic strain E-33 of Vibrio mimicus by ultrafiltration followed by gel filtration and anion-exchange column chromatography. The HAs were designated R-HA and C-HA on the basis of specific hemagglutinating activity towards rabbit erythrocytes only (R-HA) and towards chicken and rabbit erythrocytes (C-HA). Sodium dodecyl sulfate-polyacrylamide gel electrophoresis and subsequent staining with Coomassie brilliant blue revealed no detectable protein band and a single band of Mr 39,000 in the case of R-HA and C-HA, respectively. However, silver staining of the gel containing R-HA revealed the appearance of low-molecular-weight material. These two HAs differed from each other and from previously reported HA/protease in receptor specificity, molecular composition, and biochemical and immunochemical properties. No simple sugar other than glycoproteins, including mucin, inhibited hemagglutinating activities of both C-HA and R-HA. Rabbit antibody against R-HA or C-HA could agglutinate E-33 whole cells, implying a possible cell surface origin of the two HAs. The isolated E-33 lipopolysaccharide (LPS) or its polysaccharide moiety conferred biochemical and immunochemical properties identical to those of R-HA, confirming that the R-HA represents polysaccharide of LPS. The LPS preparations from heterologous strains of Vibrio mimicus and Vibrio cholerae non-O1 confirmed that the hemagglutinating ability is a common function of LPS. On the other hand, the antibody against C-HA specifically recognized a major outer membrane protein (OMP) with an Mr of around 39,000 in both homologous and heterologous strains of V. mimicus, suggesting an OMP origin of C-HA. Furthermore, the antibody recognized a major OMP with an Mr of around 37,000 in V. cholerae. Although the immunogenicity of LPS and OMP is well documented for important intestinal pathogens, the hemagglutinating properties of such attractive cell surface components are hitherto unrecognized and will definitely contribute towards understanding their role in bacterial adherence.
机译:通过超滤,然后通过凝胶过滤和阴离子交换柱色谱法,从模拟产弧菌的产毒菌株E-33的32小时培养上清液中分离出两种介导对兔红细胞凝集的血凝素(HA)。基于仅对兔红细胞(R-HA)以及对鸡和兔红细胞(C-HA)的特异性血凝活性,将HA命名为R-HA和C-HA。十二烷基硫酸钠-聚丙烯酰胺凝胶电泳以及随后的考马斯亮蓝染色显示,在R-HA和C-HA情况下,分别检测不到蛋白条带和Mr 39,000的单个条带。然而,含R-HA的凝胶的银染显示低分子量材料的外观。这两个HA在受体特异性,分子组成以及生化和免疫化学特性上彼此不同,并且与先前报道的HA /蛋白酶不同。除糖蛋白(包括粘蛋白)外,没有其他糖能抑制C-HA和R-HA的血凝活性。抗R-HA或C-HA的兔抗体可以凝集E-33全细胞,这暗示着这两个HA可能是细胞表面起源。分离的E-33脂多糖(LPS)或其多糖部分具有与R-HA相同的生化和免疫化学性质,从而证实R-HA代表LPS的多糖。从模仿弧菌和霍乱弧菌非O1的异种菌株制备LPS证实,血凝能力是LPS的共同功能。另一方面,针对C-HA的抗体特异性地识别了模仿拟约螺旋菌的同源和异源菌株中的主要外膜蛋白(OMP),其Mr约为39,000,表明C-HA的OMP起源。此外,该抗体在霍乱弧菌中识别出主要的OMP,其Mr约为37,000。尽管LPS和OMP的免疫原性已被证明对重要的肠道病原体具有重要的作用,但迄今尚未认识到这种有吸引力的细胞表面组分的血凝特性,并且肯定有助于理解它们在细菌粘附中的作用。

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