| Literature DB >> 31833228 |
Jérémy Dufloo1,2,3, Florence Guivel-Benhassine1,2, Julian Buchrieser1,2, Valérie Lorin4,5, Ludivine Grzelak1,2, Emilie Dupouy1,2, Guillaume Mestrallet1,2, Katia Bourdic6,7,8,9, Olivier Lambotte6,7,8,9, Hugo Mouquet4,5,10, Timothée Bruel1,2,10, Olivier Schwartz1,2,10.
Abstract
The effect of anti-HIV-1 antibodies on complement activation at the surface of infected cells remains partly understood. Here, we show that a subset of anti-Envelope (Env) broadly neutralizing antibodies (bNAbs), targeting the CD4 binding site and the V3 loop, triggers C3 deposition and complement-dependent cytotoxicity (CDC) on Raji cells engineered to express high surface levels of HIV-1 Env. Primary CD4 T cells infected with laboratory-adapted or primary HIV-1 strains and treated with bNAbs are susceptible to C3 deposition but not to rapid CDC. The cellular protein CD59 and viral proteins Vpu and Nef protect infected cells from CDC mediated by bNAbs or by polyclonal IgGs from HIV-positive individuals. However, complement deposition accelerates the disappearance of infected cells within a few days of culture. Altogether, our results uncover the contribution of complement to the antiviral activity of anti-HIV-1 bNAbs.Entities:
Keywords: HIV-1; broadly neutralizing antibodies; complement
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Year: 2019 PMID: 31833228 DOI: 10.15252/embr.201949351
Source DB: PubMed Journal: EMBO Rep ISSN: 1469-221X Impact factor: 8.807