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首页> 外文期刊>Molecular biology reports >Designing of an epitope-based peptide vaccine against walking pneumonia: an immunoinformatics approach
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Designing of an epitope-based peptide vaccine against walking pneumonia: an immunoinformatics approach

机译:对肺肺肺痘痘的表位肽疫苗的设计:免疫信息学方法

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Mycoplasma pneumoniae is a substantial respiratory pathogen that develops not only pneumonia but also other respiratory diseases, which mimic viral respiratory syndromes. Nevertheless, vaccine development for this pathogen delays behind as immunity correlated with protection is now predominantly unknown. In the present study, an immunoinformatics pipeline is utilized for epitope-based peptide vaccine design, which can trigger a critical immune response against M. pneumoniae. A total of 105T-cell epitopes from 12 membrane associated proteins and 7T-cell epitopes from 5 cytadherence proteins of M. pneumoniae were obtained and validated. Thus, 18 peptides with 9-mer core sequence were identified as best T-cell epitopes by considering the number of residues with >75% in favored region. Further, the crucial screening studies predicted three peptides with good binding affinity towards HLA molecules as best T-cell and B-cell epitopes. Based on this result, visualization, and dynamic simulation for the three epitopes (WIHGLILLF, VILLFLLLF, and LLAWMLVLF) were assessed. The predicted epitopes needs to be further validated for their adept use as vaccine. Collectively, the study opens up a new horizon with extensive therapeutic application against M. pneumoniae and its associated diseases.
机译:支原体肺炎是一种大量的呼吸道病,不仅发展肺炎,而且产生其他呼吸系统疾病,其模仿病毒呼吸综合征。尽管如此,这种病原体的疫苗开发后面延迟,因为与保护相关的免疫力相关,现在主要是未知数。在本研究中,免疫信息管道用于基于表位的肽疫苗设计,其可以引发针对肺炎肺炎的临界免疫应答。获得了来自12个膜相关蛋白和7克细胞表位的总共105t细胞表位,得到了来自5个肺炎的5个肺炎氏菌蛋白的表位。因此,通过考虑有利区域中具有> 75%的残留物的数量,将具有9-MEL核序列的18个肽鉴定为最佳T细胞表位。此外,关键的筛选研究预测了三种肽,其具有良好的对HLA分子具有良好的结合亲和力,作为最佳的T细胞和B细胞表位。基于此结果,评估了三个表位(Wihglillf,VillflllF和LlaWMLVLF)的可视化和动态模拟。预测表位需要​​进一步验证他们作为疫苗的熟练使用。集体,该研究开辟了一种新的地平线,具有广泛的治疗肺炎肺炎及其相关疾病。

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