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AuthorVasudevan, Karthick
AuthorD, Thirumal Kumar
AuthorS, Udhaya Kumar
AuthorSaleem, Aisha
AuthorN, Nagasundaram
AuthorR, Siva
AuthorTayubi, Iftikhar Aslam
AuthorDoss, C. George Priya
AuthorZayed, Hatem
Available date2021-11-21T07:19:28Z
Publication Date2021-11-01
Publication NameCurrent Opinion in Pharmacology
Identifierhttp://dx.doi.org/10.1016/j.coph.2021.08.015
CitationVasudevanet al. , A computational overview on Ebola virus disease, Current Opinion in Pharmacology 2021,61:28–35
URIhttp://hdl.handle.net/10576/25020
AbstractThe World Health Organization declared Ebola virus disease(EVD) as the major outbreak in the 20th century. EVD was firstidentified in 1976 in South Sudan and the Democratic Republicof the Congo. EVD was transmitted from infected fruit bats tohumans via contact with infected animal body fluids. The Ebolavirus (EBOV) has a genome size of ~18,959 bp. It encodesseven distinct proteins: nucleoprotein (NP), glycoprotein (GP),viral proteins VP24, VP30, VP35, matrix protein VP40, andpolymerase L is considered a prime target for potential antiviralstrategies. The current US FDA-approved anti-EVD vaccine,ERVERBO, and the other equally effective anti-EBOV combi-nations of three fully human monoclonal antibodies such asREGN-EB3, primarily target the envelope glycoprotein. Thiswork elaborates on the EBOV’s phylogenetic structure and thecrucial mutations associated with viral pathogenicity
Languageen
PublisherElsevier
SubjectEbola
phylogeny
drug targets
TitleA computational overview on phylogenetic characterization, pathogenic mutations, and drug targets for Ebola virus disease
TypeArticle
Pagination28-35
Volume Number61


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