Isolation and characterization of human monoclonal antibodies from individuals infected with West Nile Virus

M Throsby, C Geuijen, J Goudsmit, AQ Bakker… - Journal of …, 2006 - Am Soc Microbiol
M Throsby, C Geuijen, J Goudsmit, AQ Bakker, J Korimbocus, RA Kramer…
Journal of virology, 2006Am Soc Microbiol
ABSTRACT Monoclonal antibodies (MAbs) neutralizing West Nile Virus (WNV) have been
shown to protect against infection in animal models and have been identified as a correlate
of protection in WNV vaccine studies. In the present study, antibody repertoires from three
convalescent WNV-infected patients were cloned into an scFv phage library, and 138
human MAbs binding to WNV were identified. One hundred twenty-one MAbs specifically
bound to the viral envelope (E) protein and four MAbs to the premembrane (prM) protein …
Abstract
Monoclonal antibodies (MAbs) neutralizing West Nile Virus (WNV) have been shown to protect against infection in animal models and have been identified as a correlate of protection in WNV vaccine studies. In the present study, antibody repertoires from three convalescent WNV-infected patients were cloned into an scFv phage library, and 138 human MAbs binding to WNV were identified. One hundred twenty-one MAbs specifically bound to the viral envelope (E) protein and four MAbs to the premembrane (prM) protein. Enzyme-linked immunosorbent assay-based competitive-binding assays with representative E protein-specific MAbs demonstrated that 24/51 (47%) bound to domain II while only 4/51 (8%) targeted domain III. In vitro neutralizing activity was demonstrated for 12 MAbs, and two of these, CR4374 and CR4353, protected mice from lethal WNV challenge at 50% protective doses of 12.9 and 357 μg/kg of body weight, respectively. Our data analyzing three infected individuals suggest that the human anti-WNV repertoire after natural infection is dominated by nonneutralizing or weakly neutralizing MAbs binding to domain II of the E protein, while domain III-binding MAbs able to potently neutralize WNV in vitro and in vivo are rare.
American Society for Microbiology
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