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从腐蚀艾肯菌中部分纯化一种细菌凝集素样物质。

Partial purification of a bacterial lectinlike substance from Eikenella corrodens.

作者信息

Yamazaki Y, Ebisu S, Okada H

机构信息

Department of Endodontology and Periodontology, Osaka University, Faculty of Dentistry, Japan.

出版信息

Infect Immun. 1988 Jan;56(1):191-6. doi: 10.1128/iai.56.1.191-196.1988.

Abstract

A bacterial lectinlike substance, which is considered to participate in the adherence of Eikenella corrodens to various host cells, was purified from E. corrodens cells. The substance was extracted in 1% Triton X-100 with sonication from the cell envelope of E. corrodens 1073 and partially purified by galactosamine affinity chromatography and gel filtration chromatography based on its hemagglutination (HA) activity. The lectinlike substance was purified about 256-fold as evaluated by its specific HA activity. Sodium dodecyl sulfate-polyacrylamide gel electrophoresis of the partially purified lectinlike substance (PPL) produced a single protein band of large molecular weight when it was applied to the gel without the addition of beta-mercaptoethanol and heating. Chemical analysis showed that PPL contained 14.4 micrograms of hexose per 100 micrograms of protein and that it did not contain muramic acid, glucosamine, or 2,6-diaminopimelic acid, which are characteristic of peptidoglycans. The HA activity of PPL was inhibited by EDTA but restored by adding Ca2+. The HA activity was remarkably inhibited by sugars containing N-acetyl-D-galactosamine and D-galactose. These results indicate that the lectinlike substance on the E. corrodens cells is an essential factor for the adherence to host cells.

摘要

从腐蚀艾肯菌细胞中纯化出一种细菌凝集素样物质,该物质被认为参与了腐蚀艾肯菌对各种宿主细胞的黏附。该物质用1% Triton X - 100通过超声处理从腐蚀艾肯菌1073的细胞膜中提取,并基于其血凝(HA)活性通过半乳糖胺亲和层析和凝胶过滤层析进行部分纯化。根据其特异性HA活性评估,该凝集素样物质纯化了约256倍。当将部分纯化的凝集素样物质(PPL)在不添加β - 巯基乙醇和加热的情况下应用于凝胶时,十二烷基硫酸钠 - 聚丙烯酰胺凝胶电泳产生了一条单一的大分子蛋白带。化学分析表明,PPL每100微克蛋白质含有14.4微克己糖,且不含有肽聚糖特有的胞壁酸、氨基葡萄糖或2,6 - 二氨基庚二酸。PPL的HA活性被EDTA抑制,但通过添加Ca2 +得以恢复。HA活性被含有N - 乙酰 - D - 半乳糖胺和D - 半乳糖的糖类显著抑制。这些结果表明,腐蚀艾肯菌细胞上的凝集素样物质是其黏附宿主细胞的关键因素。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7ae4/259255/8d6928df71e3/iai00073-0211-a.jpg

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