首页> 外文期刊>Veterinary Immunology and Immunopathology >The use of binding-prediction models to identify M. bovis-specific antigenic peptides for screening assays in bovine tuberculosis
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The use of binding-prediction models to identify M. bovis-specific antigenic peptides for screening assays in bovine tuberculosis

机译:结合预测模型在牛结核分枝杆菌特异性抗原肽鉴定中的应用,以筛选牛结核病

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The identification of MHC class II-restricted antigenic peptides for inclusion into vaccines and/or as diagnostic test reagents for mycobacterial infections remains a high research priority. To expedite discovery of such peptides, numerous bioinformatic tools have been developed to predict whether a given peptide is likely to form a stable binding interaction with MHC class II molecules. However, no prediction tool dedicated to the identification of bovine MHC (BoLA) class II-restricted peptides is currently available. Using experimental immunogenicity data derived from the stimulation of whole blood of Mycobacterium bovis-infected cattle with 105 individual M. bovis-derived peptides, we have compared the ability of a novel BoLA DRB3 structure-based prediction method (Hepitom) with the human MHC class II binding predictor model ProPred in predicting peptides that induce bovine T-cell activation. When a stringent cut off for considering peptide antigenicity was applied, the sensitivities of Hepitom and ProPred in detecting immunogenic peptides were 62% and 77%, respectively. In contrast, the Hepitom model showed greater specificity, with values of 66% and 34% for Hepitom and ProPred, respectively. Using all peptides, seven out of eleven M. bovis proteins were identified as being highly immunogenic. All but one of these antigens were also identified when just the Hepitom predicted peptides were used, while only four of the seven were identified using the ProPred predicted peptides. In conclusion, we demonstrate that the Hepitom model is a useful pre-screening tool to select peptides for further immunogenicity studies in cattle without major impact on the identification of antigenic M. bovis proteins
机译:鉴定包含在疫苗中和/或作为分枝杆菌感染的诊断测试试剂的MHC II类限制性抗原肽仍然是研究的重中之重。为了加快发现这种肽,已经开发了许多生物信息学工具来预测给定的肽是否可能与II类MHC分子形成稳定的结合相互作用。但是,目前没有专门用于鉴定牛MHC(BoLA)II类限制性肽的预测工具。使用实验性免疫原性数据,该数据来源于用105种牛分枝杆菌衍生的肽刺激牛分枝杆菌感染牛的全血,我们将基于BoLA DRB3结构的新型预测方法(Hepitom)的能力与人类MHC类进行了比较II结合预测因子模型ProPred用于预测诱导牛T细胞活化的肽。当采用严格的考虑肽抗原性的标准时,Hepitom和ProPred在检测免疫原性肽方面的敏感性分别为62%和77%。相反,Hepitom模型显示出更高的特异性,Hepitom和ProPred的值分别为66%和34%。使用所有肽,在11种牛分枝杆菌蛋白中有7种被鉴定为高度免疫原性。当仅使用Hepitom预测的肽时,除一种抗原外,其他抗原都被鉴定出,而使用ProPred预测的肽则鉴定出了七种抗原中的只有四种。总之,我们证明了Hepitom模型是一种有用的预筛选工具,可以选择用于进一步进行牛免疫原性研究的肽,而对鉴定牛原性牛分枝杆菌蛋白没有重大影响

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