Design of a Novel Multi Epitope-Based Vaccine for Pandemic Coronavirus Disease (COVID-19) by Vaccinomics and Probable Prevention Strategy against Avenging Zoonotics

被引:40
作者
Ahmad, Sajjad [1 ]
Navid, Afifa [1 ]
Farid, Rabia [1 ]
Abbas, Ghulam [1 ]
Ahmad, Faisal [1 ]
Zaman, Naila [1 ]
Parvaiz, Nousheen [1 ]
Azam, Syed Sikander [1 ]
机构
[1] Quaid I Azam Univ, Natl Ctr Bioinformat NCB, Computat Biol Lab, Islamabad 45320, Pakistan
关键词
Coronavirus disease (COVID-19); Vaccinomics; Non-structural protein 8; 3C-like proteinase; Spike glycoprotein; PROTEIN-STRUCTURE; CODON USAGE; PREDICTION; ACTIVATION; REFINEMENT; EXPRESSION; SOFTWARE; IMMUNITY; TOPOLOGY; ADHESINS;
D O I
10.1016/j.ejps.2020.105387
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
The emergence and rapid expansion of the coronavirus disease (COVID-19) require the development of effective countermeasures especially a vaccine to provide active acquired immunity against the virus. This study pre- sented a comprehensive vaccinomics approach applied to the complete protein data published so far in the National Center for Biotechnological Information (NCBI) coronavirus data hub. We identified non-structural protein 8 (Nsp8), 3C -like proteinase, and spike glycoprotein as potential targets for immune responses to COVID- 19. Epitopes prediction illustrated both B -cell and T -cell epitopes associated with the mentioned proteins. The shared B and T -cell epitopes: DRDAAMQRK and QARSEDKRA of Nsp8, EDMLNPNYEDL and EFTPFDVVR of 3C - like proteinase, and VNNSYECDIPI of the spike glycoprotein are regions of high potential interest and have a high likelihood of being recognized by the human immune system. The vaccine construct of the epitopes shows stimulation of robust primary immune responses and high level of interferon gamma. Also, the construct has the best conformation with respect to the tested innate immune receptors involving vigorous molecular mechanics and solvation energy. Designing of vaccination strategies that target immune response focusing on these con- served epitopes could generate immunity that not only provide cross protection across Betacoronaviruses but additionally resistant to virus evolution.
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页数:15
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