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Importance of Antibodies to Lipopolysaccharide in Natural and Vaccine-Induced Serum Bactericidal Activity against Neisseria meningitidis Group B▿†

机译:天然和疫苗诱导的针对脑膜炎奈瑟氏球菌B组的血清杀菌活性中脂多糖抗体的重要性

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摘要

Analysis of the specificity of bactericidal antibodies in normal, convalescent, and postvaccination human sera is important in understanding human immunity to meningococcal infections and can aid in the design of an effective group B vaccine. A collection of human sera, including group C and group B convalescent-phase sera, normal sera with naturally occurring cross-reactive bactericidal activity, and some postvaccination sera, was analyzed to determine the specificity of cross-reactive bactericidal antibodies. Analysis of human sera using a bactericidal antibody depletion assay demonstrated that a significant portion of the bactericidal activity could be removed by purified lipopolysaccharide (LPS). LPS homologous to that expressed on the bactericidal test strain was most effective, but partial depletion by heterologous LPS suggested the presence of antibodies with various degrees of cross-reactivity. Binding of anti-L3,7 LPS bactericidal antibodies was affected by modification of the core structure, suggesting that these functional antibodies recognized epitopes consisting of both core structures and lacto-N-neotetraose (LNnT). When the target strain was grown with 5′-cytidinemonophospho-N-acetylneuraminic acid (CMP-NANA) to increase LPS sialylation, convalescent-phase serum bactericidal titers were decreased by only 2- to 4-fold, and most remaining bactericidal activity was still depleted by LPS. Highly sialylated LPS was ineffective in depleting bactericidal antibodies. We conclude that natural infections caused by strains expressing L3,7 LPS induce persistent, protective bactericidal antibodies and appear to be directed against nonsialylated bacterial epitopes. Additionally, subsets of these bactericidal antibodies are cross-reactive, binding to several different LPS immunotypes, which is a useful characteristic for an effective group B meningococcal vaccine antigen.
机译:在正常,恢复期和疫苗接种后的人类血清中分析杀菌抗体的特异性对于理解人类对脑膜炎球菌感染的免疫力很重要,并且可以帮助设计有效的B组疫苗。分析了一组人类血清,包括C组和B组恢复期血清,具有自然发生的交叉反应杀菌活性的正常血清以及一些接种疫苗后的血清,以确定交叉反应杀菌抗体的特异性。使用杀菌抗体耗竭测定法分析人血清表明,可以通过纯化的脂多糖(LPS)去除大部分杀菌活性。与在杀菌试验菌株上表达的LPS同源的LPS是最有效的,但是异源LPS的部分消耗表明存在具有不同程度的交叉反应性的抗体。抗L3,7 LPS杀菌抗体的结合受到核心结构修饰的影响,表明这些功能性抗体可识别由核心结构和乳酸-N-新四糖(LNnT)组成的表位。当目标菌株与5'-胞苷单磷酸-N-乙酰神经氨酸(CMP-NANA)一起生长以增加LPS唾液酸化时,恢复期的血清杀菌滴度仅降低了2到4倍,并且大多数剩余的杀菌活性仍然被LPS耗尽。高度唾液酸化的LPS在消耗杀菌抗体方面无效。我们得出结论,由表达L3,7 LPS的菌株引起的自然感染诱导了持久的保护性杀菌抗体,并且似乎针对非唾液酸化细菌表位。另外,这些杀菌抗体的子集是交叉反应的,与几种不同的LPS免疫型结合,这对于有效的B组脑膜炎球菌疫苗抗原是有用的特征。

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