In silico design and evaluation of a multiepitope vaccine targeting the nucleoprotein of Puumala orthohantavirus

Author:

Bhattacharya Kunal12ORCID,Chanu Nongmaithem Randhoni13,Jha Saurav Kumar4,Khanal Pukar5,Paudel Keshav Raj6

Affiliation:

1. Pratiksha Institute of Pharmaceutical Sciences Guwahati Assam India

2. Royal School of Pharmacy The Assam Royal Global University Guwahati Assam India

3. Faculty of Pharmaceutical Science Assam Downtown University Guwahati Assam India

4. Department of Biological Sciences and Bioengineering (BSBE) Indian Institute of Technology Kanpur Uttar Pradesh India

5. Department of Pharmacology and Toxicology KLE College of Pharmacy, Belagavi, KLE Academy of Higher Education and Research (KAHER) Belagavi India

6. Centre for Inflammation Centenary Institute and University of Technology Sydney, Faculty of Science, School of Life Sciences Sydney New South Wales Australia

Abstract

AbstractThe Puumala orthohantavirus is present in the body of the bank vole (Myodes glareolus). Humans infected with this virus may develop hemorrhagic fever accompanying renal syndrome. In addition, the infection may further lead to the failure of an immune system completely. The present study aimed to propose a possible vaccine by employing bioinformatics techniques to identify B and T‐cell antigens. The best multi‐epitope of potential immunogenicity was generated by combining epitopes. Additionally, the linkers EAAAK, AAY, and GPGPG were utilized in order to link the epitopes successfully. Further, C‐ImmSim was used to perform in silico immunological simulations upon the vaccine. For the purpose of conducting expression tests in Escherichia coli, the chimeric protein construct was cloned using Snapgene into the pET‐9c vector. The designed vaccine showed adequate results, evidenced by the global population coverage and favorable immune response. The developed vaccine was found to be highly effective and to have excellent population coverage in a number of computer‐based assessments. This work is fully dependent on the development of nucleoprotein‐based vaccines, which would constitute a significant step forward if our findings were used in developing a global vaccination to combat the Puumala virus.

Publisher

Wiley

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