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变形链球菌对结合抗体的活性释放。

Active release of bound antibody by Streptococcus mutans.

作者信息

Lee S F

机构信息

Department of Oral Biology, Faculty of Dentistry, University of Manitoba, Winnipeg, Canada.

出版信息

Infect Immun. 1995 May;63(5):1940-6. doi: 10.1128/iai.63.5.1940-1946.1995.

Abstract

Previous studies have shown that Streptococcus mutants is capable of releasing many surface protein antigens, particularly antigen P1. Antigen P1 is immunodominant and has been implicated in adherence of S. mutants to the acquired pellicles. The purpose of this study is to investigate the significance of release of this antigen by the cells. S. mutants NG8 (serotype c) was incubated with an anti-P1 rabbit immunoglobulin G (IgG) or a human colostral IgA which contains natural anti-P1 activity. Results indicated that the bound antibodies were released by the cells in a pH- and time-dependent manner. The optimal pH for release was between 6 and 8, and the release rate reached a plateau in 1 h at 37 degrees C. The release of bound antibodies was considered an active process, since heat-killed cells remained capable of antibody binding but failed to release the antibodies. The release was also dependent on the age of the culture, with early-exponential-phase cells releasing the maximum amount of bound IgG. The released IgG was isolated by polyethylene glycol precipitation and protein A-Sepharose column chromatography and found to be associated with antigen P1, indicating that the antibodies were released together with the antigen in the form of immune complexes. The binding of S. mutans by secretory IgA (SIgA) inhibited the adherence of the cells to salivary agglutinin-coated hydroxylapatite. However, when the SIgA-coated S. mutans was allowed to release the bound antibodies, the inhibitory effect of SIgA on adherence was abrogated. These results suggest that S. mutans is capable of shedding surface-bound antibodies in the form of antibody-antigen immune complexes. Such an action may be a strategy employed by the cells to counter the neutralizing effect of naturally occurring antibodies in the oral cavity.

摘要

先前的研究表明,变形链球菌能够释放多种表面蛋白抗原,尤其是抗原P1。抗原P1具有免疫显性,并且与变形链球菌黏附于获得性薄膜有关。本研究的目的是调查细胞释放这种抗原的意义。将变形链球菌NG8(血清型c)与抗P1兔免疫球蛋白G(IgG)或含有天然抗P1活性的人初乳IgA一起孵育。结果表明,结合的抗体以pH和时间依赖性方式被细胞释放。释放的最佳pH在6至8之间,在37℃下1小时内释放速率达到平台期。结合抗体的释放被认为是一个活跃的过程,因为热杀死的细胞仍能够结合抗体但无法释放抗体。释放也取决于培养物的年龄,指数生长期早期的细胞释放的结合IgG量最大。通过聚乙二醇沉淀和蛋白A-琼脂糖柱色谱法分离释放的IgG,发现其与抗原P1相关,表明抗体与抗原以免疫复合物的形式一起释放。分泌型IgA(SIgA)对变形链球菌的结合抑制了细胞对唾液凝集素包被的羟基磷灰石的黏附。然而,当允许包被SIgA的变形链球菌释放结合的抗体时,SIgA对黏附的抑制作用被消除。这些结果表明,变形链球菌能够以抗体-抗原免疫复合物的形式脱落表面结合的抗体。这种作用可能是细胞用来对抗口腔中天然存在的抗体的中和作用的一种策略。

相似文献

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Active release of bound antibody by Streptococcus mutans.变形链球菌对结合抗体的活性释放。
Infect Immun. 1995 May;63(5):1940-6. doi: 10.1128/iai.63.5.1940-1946.1995.

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