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Comparative Analysis of Two Meningococcal Immunotyping Monoclonal Antibodies by Resonant Mirror Biosensor and Antibody Gene Sequencing

机译:两种脑膜炎球菌的比较分析 共振镜生物传感器和单克隆抗体的免疫分型单克隆抗体 抗体基因测序

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摘要

Lipooligosaccharide (LOS) is a major surface component of the cell walls of Neisseria meningitidis, which is important for its roles in pathogenesis and antigenic variation, as a target for immunological typing, and as a possible vaccine component. Although the structures of many antigenic variants have been determined, routine immunological typing of these molecules remains problematic. Resonant mirror analysis was combined with gene sequencing to characterize two monoclonal antibodies (MAbs) used in typing panels that were raised against the same LOS immunotype, L3,7,9. The two MAbs (MAb 4A8-B2 and MAb 9-2-L379) were of the same immunoglobulin subtype, but while MAb 9-2-L379 was more than a 1,000-fold more sensitive in immunotyping assays of both whole meningococcal cells and purified LOS, MAb 4A8-B2 was more specific for immunotype L3,7,9. The differences in sensitivity were a consequence of MAb 9-2-L379 having a 44-fold-faster association constant than MAb 4A8-B2. Comparison of the amino acid sequences of the variable chains of the MAbs revealed that they had very similar heavy chains (81% amino acid sequence identity) but diverse light chains (54% sequence identity). The differential binding kinetics and specificities observed with these MAbs were probably due to differences in the epitopes recognized, and these were probably a consequence of the different immunization protocols used in their production.
机译:脂寡糖(LOS)是脑膜炎奈瑟氏球菌细胞壁的主要表面成分,这对于其在发病机理和抗原变异中的作用,作为免疫分型的靶标以及可能的疫苗成分非常重要。尽管已经确定了许多抗原变体的结构,但是这些分子的常规免疫分型仍然存在问题。共振镜分析与基因测序相结合,以鉴定用于针对相同LOS免疫型L3、7、9的打字面板中使用的两种单克隆抗体(MAb)。两种MAb(MAb 4A8-B2和MAb 9-2-L379)属于相同的免疫球蛋白亚型,但在整个脑膜炎球菌细胞和纯化脑膜炎球菌的免疫分型测定中,MAb 9-2-L379的敏感性高1000倍以上LOS,MAb 4A8-B2对免疫型L3,7,9更具特异性。敏感性上的差异是MAb 9-2-L379具有比MAb 4A8-B2快44倍的缔合常数的结果。 MAb可变链氨基酸序列的比较显示,它们具有非常相似的重链(81%氨基酸序列同一性),但轻链却多种多样 (54%序列同一性)。差分结合动力学和 这些单克隆抗体观察到的特异性可能是由于差异 在公认的抗原决定簇中,这些可能是由于 生产中使用的不同免疫方案。

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