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涉及B群脑膜炎奈瑟菌和大肠杆菌K1细胞表面同唾液酸多聚糖荚膜的独特分子间杀菌表位。

Unique intermolecular bactericidal epitope involving the homosialopolysaccharide capsule on the cell surface of group B Neisseria meningitidis and Escherichia coli K1.

作者信息

Jennings H J, Gamian A, Michon F, Ashton F E

机构信息

Division of Biological Sciences, National Research Council of Canada, Ottawa, Ontario.

出版信息

J Immunol. 1989 May 15;142(10):3585-91.

PMID:2469720
Abstract

The N-propionylated group B meningococcal polysaccharide mimics a unique bactericidal epitope on the surface of group B meningococci and Escherichia coli K1. This was confirmed when both the above organisms were able to absorb the bactericidal antibodies from a mouse-anti-N-propionylated group B meningococcal polysaccharide-tetanus toxoid conjugate serum. By using affinity columns it was possible to divide the conjugate antiserum into three distinct populations of both group B polysaccharide cross-reactive and non-cross-reactive antibodies, one of which contained most of the bactericidal activity. The cross-reactive (IgG1) antibodies were absorbed by an affinity column in which the group B polysaccharide was linked to the solid support by a long spacer arm, thereby isolating a population of non-cross-reactive (IgG1) antibodies. Surprisingly the above column also retained another population of non-cross-reactive (IgG2a) and (IgG2b) antibodies which contained most of the bactericidal activity. These latter antibodies were not absorbed by a similar group B polysaccharide-affinity column in which a short spacer arm was employed. Thus the above experiments not only effected a separation of highly bactericidal antibodies but also provided evidence that the long spacer arm is functional in the binding of the bactericidal antibodies to the affinity column. This indicates that the bactericidal epitope is mimicked by the group B polysaccharide in the presence of the long spacer arm, which supports the hypothesis that the epitope is polysaccharide-associated and is probably intermolecular in nature.

摘要

N-丙酰化B群脑膜炎球菌多糖模拟了B群脑膜炎球菌和大肠杆菌K1表面独特的杀菌表位。当上述两种微生物都能从小鼠抗N-丙酰化B群脑膜炎球菌多糖-破伤风类毒素结合物血清中吸收杀菌抗体时,这一点得到了证实。通过使用亲和柱,有可能将结合物抗血清分为B群多糖交叉反应性和非交叉反应性抗体的三个不同群体,其中一个群体含有大部分杀菌活性。交叉反应性(IgG1)抗体被一个亲和柱吸收,在该亲和柱中,B群多糖通过长间隔臂与固相支持物相连,从而分离出一群非交叉反应性(IgG1)抗体。令人惊讶的是,上述柱子还保留了另一群非交叉反应性(IgG2a)和(IgG2b)抗体,它们含有大部分杀菌活性。后一种抗体不被使用短间隔臂的类似B群多糖亲和柱吸收。因此,上述实验不仅实现了高杀菌活性抗体的分离,还提供了证据表明长间隔臂在杀菌抗体与亲和柱的结合中起作用。这表明在长间隔臂存在的情况下,B群多糖模拟了杀菌表位,这支持了该表位与多糖相关且可能本质上是分子间的这一假设。

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