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In Silico Identification of Novel Potential Vaccine Candidates in Streptococcus pneumoniae

机译:肺炎链球菌中新型潜在疫苗候选者的计算机鉴定

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Currently, most reverse vaccinology studies aim to identify novel proteins with signature motifs commonly found in surface exposed proteins. In the current manuscript, our objective was to computationally identify conserved, antigenic, classically or non-classically secreted proteins in pathogenic strains of Streptococcus pneumoniae. The pathogenic strains used in our analysis were TIGR4, D39, CGSP14, 19A-6, JJA, 70585, AP200, 6706B and TCH8431. PSORTb 3.0.2 was used to infer subcellular locations while SecretomeP 2.0 server was run to predict non-classically secreted proteins. Virulence was predicted using MP3 and VirulentPred webservers. A systematic workflow designed for reverse vaccinology identified 83 (45 classically secreted and 38 non-classically secreted) potential virulence factors. However, many proteins were uncharacterized. Therefore, InterProScan was run for functional annotation. Proteins failing to be annotated were filtered out leaving a set of 24 proteins (9 classically secreted and 15 non-classically secreted) as our final prediction for potential vaccine candidates. Nevertheless, predicted proteins needs to be validated in biological assays before their use as vaccines.
机译:当前,大多数反向疫苗学研究旨在鉴定具有通常在表面暴露的蛋白质中发现的特征性基序的新型蛋白质。在当前的手稿中,我们的目标是通过计算鉴定出肺炎链球菌的致病菌株中保守,抗原,经典或非经典分泌的蛋白质。我们分析中使用的致病菌株是TIGR4,D39,CGSP14、19A-6,JJA,70585,AP200、6706B和TCH8431。在运行SecretomeP 2.0服务器预测非经典分泌的蛋白质时,使用PSORTb 3.0.2推断亚细胞位置。使用MP3和VirulentPred Web服务器预测了毒力。为反向疫苗学设计的系统工作流程确定了83种(潜在分泌的45种经典分泌和38种非典型分泌的)潜在毒力因子。但是,许多蛋白质尚未鉴定。因此,运行InterProScan进行功能注释。过滤掉未注释的蛋白质,留下一组24种蛋白质(9种经典分泌的蛋白质和15种非经典分泌的蛋白质),作为我们对潜在候选疫苗的最终预测。然而,预测的蛋白质在用作疫苗之前需要在生物学分析中进行验证。

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