Engineering a multi-epitope vaccine candidate against Leishmania infantum using comprehensive Immunoinformatics methods

被引:0
|
作者
Morteza Shams
Hassan Nourmohammadi
Hamidreza Majidiani
Seyyed Ali Shariatzadeh
Ali Asghari
Mohammad Fatollahzadeh
Hamid Irannejad
机构
[1] Ilam University of Medical Sciences,Zoonotic Diseases Research Center
[2] Ilam University of Medical Sciences,Department of Internal Medicine, Shahid Mostafa Khomeini Hospital
[3] Mazandaran University of Medical Sciences,Department of Parasitology, School of Medicine
[4] Mazandaran University of Medical Sciences,Toxoplasmosis Research Center, Communicable Diseases Institute
[5] Mazandaran University of Medical Sciences,Student Research Committee
[6] Shiraz University of Medical Sciences,Department of Medical Parasitology and Mycology, School of Medicine
[7] Isfahan University of Medical Sciences,Department of Parasitology and Mycology, School of Medicine
[8] Mazandaran University of Medical Sciences,Department of Medicinal Chemistry, Faculty of Pharmacy
[9] Mazandaran University of Medical Sciences,Pharmaceutical Sciences Research Center
来源
Biologia | 2022年 / 77卷
关键词
Chimeric vaccine; Immunoinformatics;
D O I
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中图分类号
学科分类号
摘要
Visceral leishmaniasis (VL) is a severe disease with particular endemicity in over 80 countries worldwide. There is no approved human vaccine against VL in the market. This study was aimed at designing and evaluation of a multimeric vaccine candidate against Leishmania infantum through utilization of helper T lymphocyte (HTL) and cytotoxic T lymphocyte (CTL) immunodominant proteins from histone H1, KMP11, LACK and LeIF antigens. Top-ranked mouse MHC-I, MHC-II binders and CTL epitopes were predicted and joined together via spacers. Also, a TLR-4 agonist (RS-09 synthetic protein) and His-tag were added to the N- and C-terminal of the vaccine sequence, respectively. The final chimeric vaccine had a length of 184 amino acids with a molecular weight of 18.99 kDa. Physico-chemical features showed a soluble, highly-antigenic and non-allergenic candidate. Secondary and tertiary structures were predicted, and subsequent analyses confirmed the construct stability that was capable to properly interact with TLR-4/MD2 receptor. Immunoinformatics simulation displayed potent stimulation of T cell immune responses, with particular rise in IFN-γ, upon vaccination with the proposed multi-epitope candidate. In conclusion, immunoinformatics data demonstrated a highly antigenic vaccine candidate in mouse, which could develop considerable levels clearance mechanisms and other components of cellular immune profile, and can be directed for VL prophylactic purposes.
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页码:277 / 289
页数:12
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