Immunoinformatics Design of Multi-Epitope Peptide-Based Vaccine Against Schistosoma mansoni Using Transmembrane Proteins as a Target.

Rodrigo C O Sanches,Vasco A C Azevedo,Eduardo H B Maia,Sandeep Tiwari,Rodrigo Kato,Maria J F Passos,Debora O Lopes,Laís C G Ferreira,Marcelo D Lopes,Flávio M Oliveira,Alex G Taranto

doi:10.3389/fimmu.2021.621706

Abstract

Schistosomiasis remains a serious health issue nowadays for an estimated one billion people in 79 countries around the world. Great efforts have been made to identify good vaccine candidates during the last decades, but only three molecules reached clinical trials so far. The reverse vaccinology approach has become an attractive option for vaccine design, especially regarding parasites like Schistosoma spp. that present limitations for culture maintenance. This strategy also has prompted the construction of multi-epitope based vaccines, with great immunological foreseen properties as well as being less prone to contamination, autoimmunity, and allergenic responses. Therefore, in this study we applied a robust immunoinformatics approach, targeting S. mansoni transmembrane proteins, in order to construct a chimeric antigen. Initially, the search for all hypothetical transmembrane proteins in GeneDB provided a total of 584 sequences. Using the PSORT II and CCTOP servers we reduced this to 37 plasma membrane proteins, from which extracellular domains were used for epitope prediction. Nineteen common MHC-I and MHC-II binding epitopes, from eight proteins, comprised the final multi-epitope construct, along with suitable adjuvants. The final chimeric multi-epitope vaccine was predicted as prone to induce B-cell and IFN-γ based immunity, as well as presented itself as stable and non-allergenic molecule. Finally, molecular docking and molecular dynamics foresee stable interactions between the putative antigen and the immune receptor TLR 4. Our results indicate that the multi-epitope vaccine might stimulate humoral and cellular immune responses and could be a potential vaccine candidate against schistosomiasis.

Highlights

Schistosomiasis is a human parasitic disease caused by trematode parasites in the genus Schistosoma
The PSORT instability index (II) server4 was used in order to identify and select only transmembrane sequences most likely to being located in the plasma membrane [35]
In addition to check epitopes antigenicity before vaccine construction, we evaluated this parameter for the multiepitope vaccine itself

Summary

Introduction

Schistosomiasis is a human parasitic disease caused by trematode parasites in the genus Schistosoma. The World Health Organization (WHO) classifies schistosomiasis as the second most importance socioeconomic disease in the world and as the third most relevant parasitic disease regarding public health [1]. The most relevant species for human health are: Schistosoma mansoni, Schistosoma japonicum, and Schistosoma haematobium. Global areas affected by these species include: Africa and the Middle East (S. haematobium); Africa and South America (S. mansoni); China and the Philippines (S. japonicum) [4]. A recent study demonstrated that the integration of treatment and diagnosis with: health education, control of snails (intermediate host), supply of clean water, and sanitation has a great positive impact [11]. It is worth noting that Praziquantel presents little efficacy against juvenile forms of the parasite and since it is the only medicine used for mass treatment, raises legitimate concerns about drug resistance [4]

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Results

Conclusion