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In Silico Design of a Chimeric Protein Containing Antigenic Fragments of Helicobacter pylori; A Bioinformatic Approach

机译:在计算机设计中包含幽门螺杆菌抗原片段的嵌合蛋白;生物信息学方法

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摘要

Helicobacter pylori is a global health problem which has encouraged scientists to find new ways to diagnose, immunize and eradicate the H. pylori infection. In silico studies are a promising approach to design new chimeric antigen having the immunogenic potential of several antigens. In order to obtain such benefit in H. pylori vaccine study, a chimeric gene containing four fragments of FliD sequence (1-600 bp), UreB (327-334 bp),VacA (744-805 bp) and CagL(51-100 bp) which have a high density of B- and T-cell epitopes was designed. The secondary and tertiary structures of the chimeric protein and other properties such as stability, solubility and antigenicity were analyzed. The in silico results showed that after optimizing for the purpose of expression in Escherichia coli BL21, the solubility and antigenicity of the construct fragments were highly retained. Most regions of the chimeric protein were found to have a high antigenic propensity and surface accessibility. These results would be useful in animal model application and accounted for the development of an epitope-based vaccine against the H. pylori.
机译:幽门螺杆菌是一个全球性的健康问题,它鼓励科学家们寻找新的方法来诊断,免疫和根除幽门螺杆菌感染。计算机研究是设计具有几种抗原的免疫原性潜力的新嵌合抗原的有前途的方法。为了在幽门螺杆菌疫苗研究中获得这种益处,一种嵌合基因包含四个FliD序列(1-600 bp),UreB(327-334 bp),VacA(744-805 bp)和CagL(51-100)片段设计了高密度的B细胞和T细胞表位。分析了嵌合蛋白的二级和三级结构以及其他性质,例如稳定性,溶解性和抗原性。电脑分析结果表明,为达到在大肠杆菌BL21中的表达目的而进行优化后,可高度保留构建体片段的溶解性和抗原性。发现嵌合蛋白的大多数区域具有高的抗原倾向和表面可及性。这些结果在动物模型应用中将是有用的,并且可以解释针对幽门螺杆菌的基于表位的疫苗的开发。

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