A new multi-epitope peptide vaccine induces immune responses and protection against Leishmania infantum in BALB/c mice

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作者
Bahareh Vakili
Navid Nezafat
Bijan Zare
Nasrollah Erfani
Maryam Akbari
Younes Ghasemi
Mohammad Reza Rahbar
Gholam Reza Hatam
机构
[1] Shiraz University of Medical Sciences,Department of Medical Biotechnology, School of Advanced Medical Sciences and Technologies
[2] Shiraz University of Medical Sciences,Pharmaceutical Sciences Research Center
[3] Shiraz University of Medical Sciences,Department of Pharmaceutical Biotechnology, School of Pharmacy
[4] Shiraz University of Medical Sciences,Institute for Cancer Research (ICR), School of Medicine
[5] Shiraz University of Medical Sciences,Department of Parasitology
[6] Shiraz University of Medical Sciences,Basic Sciences in Infectious Diseases Research Center, School of Medicine
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关键词
Visceral leishmaniasis; Immune responses; Multi-epitope vaccines;
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摘要
Visceral leishmaniasis (VL) is a tropical and subtropical disease which is endemic in more than eighty countries around the world. Leishmania infantum is one of the main causative agents of VL disease. Currently, there is no approved-to-market vaccine for VL therapy. In this study, we evaluated cellular and humoral immune responses induced by our newly designed multi-epitope vaccine in BALB/c mice. Four antigenic proteins, including histone H1, sterol 24-c-methyltransferase (SMT), Leishmania-specific hypothetical protein (LiHy), and Leishmania-specific antigenic protein (LSAP) were chosen for the prediction of potential immunodominant epitopes. Moreover, to enhance vaccine immunogenicity, two toll-like receptors 4 (TLR4) agonists, resuscitation-promoting factors of Mycobacterium tuberculosis (RpfE and RpfB), were employed as the built-in adjuvants. Immunization with the designed multi-epitope vaccine elicited a robust Th1-type immune response, compared to other groups, as shown by increased levels of IL-2, IFN-γ, TNF-α, and IgG2a. Furthermore, a significant decrease was observed in Th-2-type-related cytokines such as IL-4 in immunized mice. The designed construct also induced a significant reduction in parasite load (p < 0.0001), conferring protection against L. infantum challenge. This study could be promising in gaining insight towards the potential of peptide epitope-based vaccines as effective protective approaches against Leishmania species.
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页码:69 / 79
页数:10
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