- Moldt, B.;
- Shibata-Koyama, M.;
- Rakasz, E. G;
- Schultz, N.;
- Kanda, Y.;
- Dunlop, D. C;
- Finstad, S. L;
- Jin, C.;
- Landucci, G.;
- Alpert, M. D;
- Dugast, A.-S.;
- Parren, P. W. H. I;
- Nimmerjahn, F.;
- Evans, D. T;
- Alter, G.;
- Forthal, D. N;
- Schmitz, J. E;
- Iida, S.;
- Poignard, P.;
- Watkins, D. I;
- Hessell, A. J;
- Burton, D. R
Eliciting neutralizing antibodies is thought to be a key activity of a vaccine against human immunodeficiency virus (HIV). However, a number of studies have suggested that in addition to neutralization, interaction of IgG with Fc gamma receptors (FcγR) may play an important role in antibody-mediated protection. We have previously obtained evidence that the protective activity of the broadly neutralizing human IgG1 anti-HIV monoclonal antibody (MAb) b12 in macaques is diminished in the absence of FcγR binding capacity. To investigate antibody-dependent cellular cytotoxicity (ADCC) as a contributor to FcγR-associated protection, we developed a nonfucosylated variant of b12 (NFb12). We showed that, compared to fully fucosylated (referred to as wild-type in the text) b12, NFb12 had higher affinity for human and rhesus macaque FcγRIIIa and was more efficient in inhibiting viral replication and more effective in killing HIV-infected cells in an ADCC assay. Despite these more potent in vitro antiviral activities, NFb12 did not enhance protection in vivo against repeated low-dose vaginal challenge in the simian-human immunodeficiency virus (SHIV)/macaque model compared to wild-type b12. No difference in protection, viral load, or infection susceptibility was observed between animals given NFb12 and those given fully fucosylated b12, indicating that FcγR-mediated activities distinct from FcγRIIIa-mediated ADCC may be important in the observed protection against SHIV challenge.