The envelope protein of dengue virus (DENV) is a primary target of the humoral immune response. The domain III of the DENV envelope protein (EDIII) is known to be the target of multiple potently neutralizing antibodies. One such antibody is 3H5, a mouse antibody that binds strongly to EDIII and potently neutralizes DENV serotype 2 (DENV-2) with unusually minimal antibody-dependent enhancement (ADE). To selectively display the binding epitope of 3H5, we strategically modified DENV-2 EDIII by shielding other known epitopes with engineered N-glycosylation sites. The modifications resulted in a glycosylated EDIII antigen termed "EDIII mutant N". This antigen was successfully used to sift through a dengue-immune scFv-phage library to select for scFv antibodies that bind to or closely surround the 3H5 epitope. The selected scFv antibodies were expressed as full-length human antibodies and showed potent neutralization activity to DENV-2 with low or negligible ADE resembling 3H5. These findings not only demonstrate the capability of the N-glycosylated EDIII mutant N as a tool to drive an epitope-directed antibody selection campaign but also highlight its potential as a dengue immunogen. This glycosylated antigen shows promise in focusing the antibody response toward a potently neutralizing epitope while reducing the risk of antibody-dependent enhancement.
[1]Natl Sci & Technol Dev Agcy NSTDA, Med Mol Biotechnol Res Grp, Mol Biol Dengue & Flaviviruses Res Team, Pathum Thani 12120, Thailand.
[2]Mahidol Univ, Siriraj Ctr Res Excellence Dengue & Emerging Patho, Bangkok 10700, Thailand.
[3]Natl Sci & Technol Dev Agcy NSTDA, Natl Ctr Genet Engn & Biotechnol BIOTEC, Med Biotechnol Res Unit, Pathum Thani 12120, Thailand.
[4]Mahidol Univ, Fac Med, Div Dengue Hemorrhag Fever Res, Siriraj Hosp, Bangkok 10700, Thailand.
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