| Literature DB >> 32053790 |
Surender Khurana1, Supriya Ravichandran2, Megan Hahn2, Elizabeth M Coyle2, Spencer W Stonier3, Samantha E Zak3, Jason Kindrachuk4, Richard T Davey5, John M Dye3, Daniel S Chertow6.
Abstract
Evolution of antibody repertoire against the Ebola virus (EBOV) proteome was characterized in an acutely infected patient receiving supportive care alone to elucidate virus-host interactions over time. Differential kinetics are observed for IgM-IgG-IgA epitope diversity, antibody binding, and affinity maturation to EBOV proteins. During acute illness, antibodies predominate to VP40 and glycoprotein (GP). At day 13 of clinical illness, a marked increase in antibody titers to most EBOV proteins and affinity maturation to GP is associated with rapid decline in viral replication and illness severity. At one year, despite undetectable virus, a diverse IgM repertoire against VP40 and GP epitopes is observed suggesting occult viral persistence. Rabbit immunization experiments identify key immunodominant sites of GP, while challenge studies in mice found these epitopes induce EBOV-neutralizing antibodies and protect against lethal EBOV challenge. This study reveals markers of viral persistence and provides promising approaches for development and evaluation of vaccines and therapeutics. Published by Elsevier Inc.Entities:
Keywords: Ebola; GFPDL; GP; affinity; antibody; correlates of protection; epitope mapping; genome-fragment phage display library; glycoprotein; immune response; infection; neutralization; vaccine; virus
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Year: 2020 PMID: 32053790 PMCID: PMC7071344 DOI: 10.1016/j.chom.2020.01.001
Source DB: PubMed Journal: Cell Host Microbe ISSN: 1931-3128 Impact factor: 21.023