首页> 外文期刊>Infection and immunity >Moraxella catarrhalis Outer Membrane Protein CD Elicits Antibodies That Inhibit CD Binding to Human Mucin and Enhance Pulmonary Clearance of M. catarrhalis in a Mouse Model
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Moraxella catarrhalis Outer Membrane Protein CD Elicits Antibodies That Inhibit CD Binding to Human Mucin and Enhance Pulmonary Clearance of M. catarrhalis in a Mouse Model

机译:卡他莫拉菌外膜蛋白CD诱导抗体抑制CD与人粘蛋白结合并增强小鼠模型中卡他莫拉菌的肺通透性

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The outer membrane protein CD of Moraxella catarrhalis is considered to be a potential vaccine antigen against Moraxella infection. We purified the native CD from isolate O35E, administered it to mice, and detected considerable titers of anti-CD antibodies. Anti-CD sera were cross-reactive towards six different M. catarrhalis isolates and promoted bacterial clearance of O35E in a pulmonary challenge model. To circumvent the difficulty of generating large quantities of CD from M. catarrhalis for vaccine use, the CD gene from O35E was cloned into Escherichia coli, and the recombinant CD, expressed without a signal sequence or fusion tags, represented ~70% of the total E. coli proteins. The recombinant CD formed inclusion bodies that were solubilized with 6 M urea and then purified by ion-exchange chromatography, a procedure that produced soluble CD of high purity and yield. Mice immunized with the purified recombinant CD had significant titers of anti-CD antibodies that were cross-reactive towards 24 different M. catarrhalis isolates. Upon challenge, these mice showed enhanced bacterial clearance of both O35E and a heterologous M. catarrhalis isolate, TTA24. In an in vitro assay, antisera to either the native or the recombinant CD inhibited the binding activity of CD to human tracheobronchial mucin in a serum concentration-dependent manner, and the extent of inhibition appeared to correlate with the corresponding anti-CD antibody titer and whole-cell enzyme-linked immunosorbent assay titer. Our results demonstrate that the recombinant CD is a promising vaccine candidate for preventing Moraxella infection.
机译:卡他莫拉氏菌的外膜蛋白CD被认为是针对莫拉氏菌感染的潜在疫苗抗原。我们从分离物O35E中纯化了天然CD,将其施用于小鼠,并检测到相当滴度的抗CD抗体。抗CD血清对6种不同的M交叉反应。肺部攻击模型中,粘膜炎菌分离并促进了O35E的细菌清除。为了避免从 M生成大量CD的困难。粘膜炎疫苗,将O35E的CD基因克隆到大肠埃希菌中,表达没有信号序列或融合标签的重组CD约占总的70%。 > E。大肠杆菌蛋白。重组CD形成包涵体,将其用6 M尿素溶解,然后通过离子交换色谱法纯化,该程序可生产高纯度和高产率的可溶性CD。用纯化的重组CD免疫的小鼠具有明显的抗CD抗体效价,这些抗体对24种不同的M交叉反应。卡他氏菌分离株。攻击后,这些小鼠表现出增强的O35E和异源 M细菌清除率。粘膜炎隔离株TTA24。在体外测定中,天然或重组CD的抗血清以血清浓度依赖性的方式抑制CD与人气管支气管粘蛋白的结合活性,并且抑制程度似乎与相应的抗CD抗体效价和全细胞酶联免疫吸附测定效价。我们的结果表明重组CD是预防 Moraxella 感染的有希望的疫苗候选者。

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