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抗体介导的对抗埃立克体属病原体的免疫的分子基础涉及串联重复蛋白中的种特异性线性表位。

Molecular basis of antibody mediated immunity against Ehrlichia chaffeensis involves species-specific linear epitopes in tandem repeat proteins.

机构信息

Department of Pathology, University of Texas Medical Branch, Galveston, TX 77555-0609, United States.

出版信息

Microbes Infect. 2012 Oct;14(12):1054-63. doi: 10.1016/j.micinf.2012.05.012. Epub 2012 May 29.

Abstract

Humoral immune mechanisms are an important component of protective immunity to Ehrlichia species. However, the molecular basis of antibody mediated immunity is not completely defined, and the role of most molecularly characterized major immunoreactive proteins is unknown. In previous studies, we mapped major species-specific continuous epitopes in three surface exposed and secreted tandem repeat proteins (TRP32, TRP47 and TRP120). In this study, we report that protection is provided by antibodies against these molecularly defined TRP epitopes using in vitro and in vivo models. Protection was demonstrated in vitro after prophylactic and therapeutic administration of epitope-specific anti-TRP antibodies, suggesting that the protective mechanisms involve extracellular and intracellular antibody-mediated effects. In vivo passive transfer of individual epitope-specific TRP sera significantly reduced the ehrlichial load and splenomegaly, and protected mice against lethal infection. Moreover, the combination of antibodies to all three TRPs provided enhanced reduction in ehrlichial load similar to that of Ehrlichia chaffeensis immune sera. IgG1 was the predominant antibody isotype in the epitope-specific TRP mouse sera. These results demonstrate that antibodies against linear epitopes in TRP32, TRP47 and TRP120 are protective during E. chaffeensis infection and involves extracellular and intracellular antibody-mediated mechanisms.

摘要

体液免疫机制是保护人体免受埃立克体属感染的重要组成部分。然而,抗体介导的免疫的分子基础尚未完全确定,并且大多数分子特征明确的主要免疫反应蛋白的作用也尚不清楚。在之前的研究中,我们在三种表面暴露和分泌串联重复蛋白(TRP32、TRP47 和 TRP120)中定位了主要的种特异性连续表位。在这项研究中,我们报告了使用体外和体内模型针对这些分子定义的 TRP 表位的抗体提供的保护作用。在预防性和治疗性给予表位特异性抗-TRP 抗体后,在体外证明了保护作用,这表明保护机制涉及细胞外和细胞内抗体介导的作用。在体内被动转移个体表位特异性 TRP 血清可显著降低埃立克体负荷和脾肿大,并可保护小鼠免受致死性感染。此外,针对所有三种 TRP 的抗体的组合提供了增强的埃立克体负荷减少,类似于对埃立克体 chaffeensis 免疫血清的减少。在针对 TRP 的小鼠血清中,IgG1 是主要的抗体同种型。这些结果表明,针对 TRP32、TRP47 和 TRP120 线性表位的抗体在 E. chaffeensis 感染期间具有保护作用,并且涉及细胞外和细胞内抗体介导的机制。

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