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细粒棘球蚴肌动蛋白作为囊型包虫病疫苗候选分子的生物信息学特征和免疫表位分析

Bioinformatics features and immunogenic epitopes of Echinococcus granulosus Myophilin as a promising target for vaccination against cystic echinococcosis.

机构信息

Zoonotic Diseases Research Center, Ilam University of Medical Sciences, Ilam, Iran.

Clinical Research Development Center, "The Persian Gulf Martyrs" Hospital, Bushehr, University of Medical Sciences, Bushehr, Iran.

出版信息

Infect Genet Evol. 2021 Apr;89:104714. doi: 10.1016/j.meegid.2021.104714. Epub 2021 Jan 9.

Abstract

Cystic echinococcosis (CE) is a neglected zoonosis especially in underdeveloped countries around the world. Hence, immunization strategies are beneficial to avert the infection. The present investigation was aimed to predict the primary biochemical characteristics of the EgMyophilin and its potential B-cell and human leukocyte antigen (HLA)-binding epitopes as a promising vaccine candidate. Different web servers were used to predict physico-chemical, antigenic and allergenic profiles, transmembrane domain, subcellular localization, post-translational modification (PTM) sites, secondary and 3D structure, tertiary model refinement and validations. B-cell and HLA-binding epitopes were predicted and screened in terms antigenicity, allergenicity, solubility (B-cell) or hydrophobicity (T-cell). The 89.82 KDa protein was non-allergenic, hydrophilic, stable, with improved thermotolerance and 94 post-translational modification sites. The secondary structure included 42.94% alpha helix, 42.82% random coil and 41.23% extended strand. Based on Ramachandran plot output for refined model, 96.2%, 99.5%, and 0.45% of amino acid residues were incorporated in the favored, allowed, and outlier regions of the refined model, respectively. After epitope screening, four B-cell and five HLA-binding epitopes possessed the highest antigenic index in the protein sequence. This paper is a premise for further researches, and provides insights for the development of a suitable vaccine against CE. More empirical studies are required using the EgMyophilin alone or in combination with other antigens/epitopes in the future.

摘要

包虫病(CE)是一种被忽视的人畜共患寄生虫病,尤其在世界范围内的欠发达国家更为严重。因此,免疫策略有利于预防感染。本研究旨在预测EgMyophilin 的主要生化特性及其潜在的 B 细胞和人类白细胞抗原(HLA)结合表位,作为一种有前途的疫苗候选物。不同的网络服务器被用于预测理化特性、抗原性和变应原性、跨膜结构域、亚细胞定位、翻译后修饰(PTM)位点、二级和 3D 结构、三级模型细化和验证。B 细胞和 HLA 结合表位根据抗原性、变应原性、可溶性(B 细胞)或疏水性(T 细胞)进行预测和筛选。该 89.82kDa 蛋白是非变应原性的、亲水的、稳定的,具有提高的热稳定性和 94 个翻译后修饰位点。二级结构包括 42.94%的α螺旋、42.82%的无规卷曲和 41.23%的伸展链。基于细化模型的 Ramachandran 图输出,96.2%、99.5%和 0.45%的氨基酸残基分别位于细化模型的偏好区域、允许区域和异常区域。在表位筛选后,四个 B 细胞和五个 HLA 结合表位在蛋白质序列中具有最高的抗原指数。本文为进一步的研究提供了前提,并为开发针对包虫病的合适疫苗提供了思路。未来需要使用 EgMyophilin 单独或与其他抗原/表位联合进行更多的实证研究。

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