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In Vitro and In Vivo Neutralization of the Relapsing Fever Agent Borrelia hermsii with Serotype-Specific Immunoglobulin M Antibodies

机译:血清型特异性免疫球蛋白M抗体对退热试剂博氏疏螺旋体的体内和体外中和

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摘要

The antigenic variation of the relapsing fever agent Borrelia hermsii is associated with changes in the expression of the Vlp and Vsp outer membrane lipoproteins. To investigate whether these serotype-defining proteins are the target of a neutralizing and protective antibody response, monoclonal antibodies were produced from spleens of infected mice just after clearance of serotype 7 cells from the blood. Two immunoglobulin M monoclonal antibodies, H7-7 and H7-12, were studied in detail. Both antibodies specifically agglutinated serotype 7 cells and inhibited their growth in vitro. Administered to mice before or after infection, both antibodies provided protection against infection or substantially reduced the number of spirochetes in the blood of mice after infection. Whereas antibody H7-12 bound to Vlp7 in Western blotting, enzyme-linked immunosorbent assay, and immunoprecipitation assays, as well as to whole cells in other immunoassays, antibody H7-7 only bound to wet, intact cells of serotype 7. Antibody H7-7 selected against cells expressing Vlp7 in vitro and in vivo, an indication that Vlp7 was a conformation-sensitive antigen for the antibody. Vaccination of mice with recombinant Vlp7 with adjuvant elicited antibodies that bound to fixed whole cells of serotype 7 and to Vlp7 in Western blots, but these antibodies did not inhibit the growth of serotype 7 in vitro and did not provide protection against an infectious challenge with serotype 7. The study established that a Vlp protein was the target of a neutralizing antibody response, and it also indicated that the conformation and/or the native topology of Vlp were important for eliciting that immunity.
机译:复发性发烧博氏疏螺旋体的抗原变异与Vlp和Vsp外膜脂蛋白表达的变化有关。为了研究这些血清型定义蛋白是否是中和和保护性抗体应答的靶标,在从血液中清除血清型7细胞后,从感染小鼠的脾脏中产生单克隆抗体。详细研究了两种免疫球蛋白M单克隆抗体H7-7和H7-12。两种抗体都特异性凝集血清7型细胞,并在体外抑制其生长。在感染之前或之后对小鼠施用,两种抗体均提供了针对感染的保护或大大减少了感染后小鼠血液中螺旋体的数量。抗体H7-12在Western印迹,酶联免疫吸附测定和免疫沉淀测定中与Vlp7结合,而在其他免疫测定中与全细胞结合,而抗体H7-7仅与7型血清干完整细胞结合。针对体外和体内表达Vlp7的细胞选择了7种,这表明Vlp7是抗体的构象敏感抗原。用佐剂诱导的重组Vlp7小鼠疫苗免疫西方血清中与血清7型固定全细胞和Vlp7结合的抗体,但这些抗体在体外不能抑制血清7型的生长,也不能提供针对血清型传染性攻击的保护作用7.研究确定Vlp蛋白是中和抗体反应的靶标,并且还表明Vlp的构象和/或天然拓扑对于引发这种免疫力很重要。

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