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用于疫苗开发的人轮状病毒VP7基因型G9表位的计算机模拟表征

In Silico Characterization of Epitopes from Human Rotavirus VP7 Genotype G9 Design for Vaccine Development.

作者信息

Jalilian Shahram, Teimoori Ali, Makvandi Manoochehr

机构信息

Infectious and Tropical Diseases Research Center, Health Research Institute, Ahvaz Jundishapur University of Medical Sciences, Ahvaz, Iran AND Department of Virology, School of Medicine, Ahvaz Jundishapur University of Medical Sciences, Ahvaz, Iran.

出版信息

Iran J Allergy Asthma Immunol. 2019 Nov 10;18(6):664-670. doi: 10.18502/ijaai.v18i6.2179.

Abstract

Acute gastroenteritis caused by Rotavirus remains the leading cause of child mortality worldwide. Rotavirus genotype G9 circulates in humans throughout the world. Antibodies against the outer glycoproteins VP7 and VP4 Rotavirus capsid are the main neutralization antibodies in the vaccine assessment. This study aimed to select an epitope to evoke T and B cells' response, as a favorable candidate for vaccine development using in Silico evaluation. In the present study, Rotavirus genotypes were determined in 100 stools specimens collected from children with acute diarrhea. The results showed predominant G genotype, G9 (38.5%) followed by G2 (22.9%), G1 (16.5%), G12 (11.4%), G4 (6.4%), and G3 (4.3%). The G9 was dominant in this study and other regions of Iran; thus, this study was conducted to select an epitope from Rotavirus genotype G9 as a promising epitope candidate for future vaccine development. For this reason, several works including a complete sequence of VP7 G9, phylogenetic analysis, Prediction of Protein Structure, Physicochemical Properties of Protein and Epitope prediction were carried out. The outcomes of this study revealed that the complete sequence of VP7 (G9) was comprised of 1062 nt with 326 amino acids (accession number MH824633). The selected epitope contained amino acid sequence of STLCLYYPTEASTQIGDTEWKN with the best score for T and B cells response. Based on data of computational biology, the selected epitope can optimistically have considered as an epitope candidate for rotavirus vaccine development.

摘要

轮状病毒引起的急性肠胃炎仍是全球儿童死亡的主要原因。轮状病毒G9基因型在全球人类中传播。针对轮状病毒衣壳外糖蛋白VP7和VP4的抗体是疫苗评估中的主要中和抗体。本研究旨在通过计算机评估选择一个能引发T细胞和B细胞反应的表位,作为疫苗开发的理想候选物。在本研究中,对从急性腹泻儿童收集的100份粪便样本进行了轮状病毒基因型测定。结果显示主要的G基因型为G9(38.5%),其次是G2(22.9%)、G1(16.5%)、G12(11.4%)、G4(6.4%)和G3(4.3%)。G9在本研究及伊朗其他地区占主导地位;因此,本研究旨在从轮状病毒G9基因型中选择一个表位,作为未来疫苗开发的有前景的表位候选物。为此,开展了多项工作,包括VP7 G9的完整序列、系统发育分析、蛋白质结构预测、蛋白质理化性质和表位预测。本研究结果显示,VP7(G9)的完整序列由1062个核苷酸组成,含326个氨基酸(登录号MH824633)。所选表位包含氨基酸序列STLCLYYPTEASTQIGDTEWKN,对T细胞和B细胞反应的评分最佳。基于计算生物学数据,所选表位有望被视为轮状病毒疫苗开发的表位候选物。

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