利什曼病主要 gp46 蛋白的免疫形式分析和利什曼病疫苗的潜在靶标。

IF 1.2 Q4 PHARMACOLOGY & PHARMACY
Mohammad Reza Hafezi Ahmadi, Mina Mamizadeh, Davood Siamian, Mehdi Ali Asghari Touyeh, Morteza Shams, Yasaman Rashidi
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引用次数: 0

摘要

背景:皮肤利什曼病(CL皮肤利什曼病(CL)是一种寄生虫病,给旧世界国家带来了沉重负担:本研究预测了利什曼原虫主要抗原蛋白 gp46 的一些主要生化特性以及与人类和小鼠 MHC 等位基因具有特异性结合能力的 IFN-γ 诱导表位:使用多个在线服务器预测理化性状、过敏性、抗原性、跨膜域和信号肽、亚细胞定位、翻译后修饰(PTMs)、二级和三级结构、三级模型提炼和验证。此外,还利用 IEDB 网络服务器预测了小鼠/人类细胞毒性 T 淋巴细胞(CTL)和辅助性 T 淋巴细胞(HTL)表位:33.25 kDa 蛋白稳定、亲水性强、抗原性强、无过敏性、耐热性强,有 45 个 PTM 位点。二级结构包括一个随机线圈,其次是延伸的链和螺旋。基于拉马钱德兰分析法对完善后的模型进行了分析,结果显示,在最有利、额外允许、慷慨允许和不允许区域的残基分别占 73.1%、21.6%、3.4% 和 1.9%。表位筛选结果表明,有 4 个 HTL 表位针对看似具有保护性的 HLA 等位基因,5 个 HTL 表位针对 HLA 参考集,3 个人类 CTL 表位和一些小鼠 MHC 限制表位:本文深入探讨了大肠杆菌 gp46 蛋白作为候选疫苗的生物信息学特征。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Immunoinformatic Analysis of Leishmania Major gp46 Protein and Potential Targets for Vaccination against Leishmaniasis.

Background: Cutaneous leishmaniasis (CL) is a parasitic disease with a significant burden in the Old World countries.

Objective: In the current study, some of the primary biochemical properties and IFN-γ inducing epitopes with specific binding capacity to human and mouse MHC alleles were predicted for Leishmania major gp46 antigenic protein.

Methods: Several online servers were used to predict physico-chemical traits, allergenicity, antigenicity, transmembrane domain and signal peptide, subcellular localization, post-translational modifications (PTMs), secondary and tertiary structures, tertiary model refining with validations. Also, IEDB web server was used to predict mouse/human cytotoxic T-lymphocyte (CTL) and helper T-lymphocyte (HTL) epitopes.

Results: The 33.25 kDa protein was stable, hydrophilic, antigenic, while non-allergenic, with enhanced thermotolerance and 45 PTM sites. The secondary structure encompassed a random coil, followed by extended strands and helices. Ramachandran-based analysis of the refined model showed 73.1%, 21.6%, 3.4% and 1.9% of residues in the most favored, additional allowed, generously-allowed and disallowed regions, respectively. Epitope screening demonstrated 4 HTL epitopes against seemingly protective HLA alleles, 5 HTL epitopes against the HLA reference set, 3 human CTL epitopes and a number of mouse MHC-restricted epitopes.

Conclusion: This paper provides insights into the bioinformatics characteristics of the L. major gp46 protein as a promising vaccine candidate.

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CiteScore
4.30
自引率
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