๐ Characterization of neutralizing monoclonal antibodies recognizing a 15-residues epitope on the spike protein HR2 region of severe acute respiratory syndrome coronavirus (SARS-CoV)
The spike (S) glycoprotein is thought to play a complex and central role in the biology and pathogenesis of SARS coronavirus infection. In this study, a recombinant protein (rS268, corresponding to residues 268-1255 of SARS-CoV S protein) was expressed in Escherichia coli and was purified to near homogeneity. After immunization with rS268, S protein-specific BALB/c antisera and mAbs were induced and confirmed using ELISA, Western blot and IFA. Several BALB/c mAbs were found to be effectively to neutralize the infection of Vero E6 cells by SARS-CoV in a dose-dependent manner. Systematic epitope mapping showed that all these neutralizing mAbs recognized a 15-residues peptide (CB-119) corresponding to residues 1143-1157 (SPDVDLGDISGINAS) that was located to the second heptad repeat (HR2) region of the SARS-CoV spike protein. The peptide CB-119 could specifically inhibit the interaction of neutralizing mAbs and spike protein in a dose-dependent manner. Further, neutralizing mAbs, but not control mAbs, could specifically interact with CB-119 in a dose-dependent manner. Results implicated that the second heptad repeat region of spike protein could be a good target for vaccine development against SARS-CoV. ยฉ 2005 National Science Council.
keywords
๐ dose-dependent manner (15)
๐ spike protein (353)
๐ coronavirus infection (270)
๐ heptad repeat (55)
author
๐ค Lai, Szu Chia
๐ค Chong, Pele Choi Sing
๐ค Yeh, Chia Tsui
๐ค Liu, Levent Shih Jen
๐ค Jan, Jia Tsrong
๐ค Chi, Hsiang Yun
๐ค Liu, Hwan Wun
๐ค Chen, Ann
๐ค Wang, Yeau Ching
year
โฐ 2005
issn
๐ 10217770 14230127
volume
12
number
5
page
711-727
citedbycount
16
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