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Tuberculosis vaccine with high predicted population coverage and compatibility with modern diagnostics

机译:预测人群覆盖率高且与现代诊断方法兼容的结核疫苗

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摘要

A central goal in vaccine research is the identification of relevant antigens. The Mycobacterium tuberculosis chromosome encodes 23 early secretory antigenic target (ESAT-6) family members that mostly are localized as gene pairs. In proximity to five of the gene pairs are ESX secretion systems involved in the secretion of the ESAT-6 family proteins. Here, we performed a detailed and systematic investigation of the vaccine potential of five possible Esx dimer substrates, one for each of the five ESX systems. On the basis of gene transcription during infection, immunogenicity, and protective capacity in a mouse aerosol challenge model, we identified the ESX dimer substrates EsxD-EsxC, ExsG-EsxH, and ExsW-EsxV as the most promising vaccine candidates and combined them in a fusion protein, H65. Vaccination with H65 gave protection at the level of bacillus Calmette–Guérin, and the fusion protein exhibited high predicted population coverage in high endemic regions. H65 thus constitutes a promising vaccine candidate devoid of antigen 85 and fully compatible with current ESAT-6 and culture filtrate protein 10-based diagnostics.
机译:疫苗研究的主要目标是鉴定相关抗原。结核分枝杆菌染色体编码23个早期分泌性抗原靶标(ESAT-6)家族成员,这些家族成员大多定位为基因对。与五个基因对相邻的是参与ESAT-6家族蛋白分泌的ESX分泌系统。在这里,我们对五种可能的Esx二聚体底物的疫苗潜力进行了详细而系统的研究,每种五种ESX系统中的一种均适用。根据小鼠气溶胶攻击模型中感染,免疫原性和保护能力期间的基因转录,我们确定了ESX二聚体底物EsxD-EsxC,ExsG-EsxH和ExsW-EsxV是最有前途的候选疫苗,并将它们组合在一起融合蛋白,H65。用H65疫苗接种可在卡介苗的水平上提供保护,融合蛋白在高流行地区显示出较高的预测人群覆盖率。因此,H65构成了一种有希望的疫苗候选物,不含抗原85,并且与当前的ESAT-6和基于培养物滤液蛋白10的诊断方法完全兼容。

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