Molecular and biological characterization of human monoclonal antibodies binding to the spike and nucleocapsid proteins of severe acute respiratory syndrome coronavirus.

Authors :: Brink, E.N. (Edward) van den
Meulen, J. (Jan) ter
Cox, F. (Freek)
Jongeneelen, M.A. (Mandy)
Thijsse, A. (Alexandra)
Throsby, M. (Mark)
Marissen, W.E. (Wilfred)
Rood, P.M. (Pauline)
Bakker, A.B. (Alexander)
Gelderblom, H.R. (Hans)
Martina, B.E.E. (Byron)
Osterhaus, A.D.M.E. (Albert)
Preiser, W. (Wolfgang)
Doerr, H.W.
Kruif, J. (John) de
Goudsmit, J. (Jaap)
Brink, E.N. (Edward) van den
Meulen, J. (Jan) ter
Cox, F. (Freek)
Jongeneelen, M.A. (Mandy)
Thijsse, A. (Alexandra)
Throsby, M. (Mark)
Marissen, W.E. (Wilfred)
Rood, P.M. (Pauline)
Bakker, A.B. (Alexander)
Gelderblom, H.R. (Hans)
Martina, B.E.E. (Byron)
Osterhaus, A.D.M.E. (Albert)
Preiser, W. (Wolfgang)
Doerr, H.W.
Kruif, J. (John) de
Goudsmit, J. (Jaap)
Publication Year :: 2005
Abstract: Human monoclonal antibodies (MAbs) were selected from semisynthetic antibody phage display libraries by using whole irradiated severe acute respiratory syndrome (SARS) coronavirus (CoV) virions as target. We identified eight human MAbs binding to virus and infected cells, six of which could be mapped to two SARS-CoV structural proteins: the nucleocapsid (N) and spike (S) proteins. Two MAbs reacted with N protein. One of the N protein MAbs recognized a linear epitope conserved between all published human and animal SARS-CoV isolates, and the other bound to a nonlinear N epitope. These two N MAbs did not compete for bindi

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