Recombinant human monoclonal antibodies to human cytomegalovirus glycoprotein B neutralize virus in a complement-dependent manner |
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Authors: | Akane Ohta Ayano Fujita Tsugiya Murayama Yoshitaka Iba Yoshikazu Kurosawa Tetsushi Yoshikawa Yoshizo Asano |
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Affiliation: | a21st Century COE Research Center, Toyoake, Aichi, Japan;bDivision of Immunology, Institute for Comprehensive Medical Science, Fujita Health University, Toyoake, Aichi, Japan;cDepartment of Pediatrics, Fujita Health University School of Medicine, Toyoake, Aichi, Japan;dDepartment of Microbiology and Immunology, Faculty of Pharmaceutical Sciences, Hokuriku University, Kanazawa, Japan |
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Abstract: | ![]() Human antibodies specific for HCMV are currently considered as potential anti-HCMV therapeutic agents. In this study, we used a combinatorial human antibody library to isolate and characterize complete human monoclonal antibodies that effectively neutralize HCMV in a complement-dependent manner. One hundred and six clones were isolated in two independent screens using HCMV virions and recombinant glycoprotein B, gB654, as antigens. All of the clones recognized the same molecule gB and were classified into 14 groups based on the amino acid sequence of the VH region. Seven representative clones from these 14 groups had a strong gB654 binding affinity by surface plasmon resonance (SPR). A pairwise binding competition analysis suggested that there were three groups based on differences in the gB recognition sites. Although Fab fragments of the seven groups showed strong affinity for gB, none of the Fab fragments neutralized HCMV infectivity in vitro. In contrast, complete human IgG1 antibodies of at least three groups neutralized HCMV in a complement-dependent manner. These data suggest that potent therapeutic antibodies can be obtained from a human antibody library, including most of the functional antibodies that mediate humoral immunity to the selected pathogen. |
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Keywords: | HCMV Human antibody Phage display Antiviral agents |
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