Virologic effects of broadly neutralizing antibody VRC01 administration during chronic HIV-1 infection

Lynch, Rebecca M.; Boritz, Eli; Coates, Emily E.; DeZure, Adam; Madden, Patrick; Costner, Pamela; Enama, Mary E.; Plummer, Sarah H.; Holman, LaSonji A.; Hendel, Cynthia S.; Gordon, Ingelise J.; Casazza, Joseph P.; Conan-Cibotti, Michelle; Migueles, Stephen A.; Tressler, Randall; Bailer, Robert T.; McDermott, Adrian B.; Narpala, Sandeep; O’Dell, Sijy; Wolf, Gideon; Lifson, Jeffrey D.; Freemire, Brandie A.; Gorelick, Robert J.; Pandey, Janardan P.; Mohan, Sarumathi; Chomont, Nicolas; Fromentin, Rémi; Chun, Tae‐Wook; Fauci, Anthony S.; Schwartz, Richard; Koup, Richard A.; Douek, Daniel C.; Hu, Zonghui; Capparelli, Edmund V.; Graham, Barney S.; Mascola, John R.; Ledgerwood, Julie E.; Team, Vrc Study

doi:10.1126/scitranslmed.aad5752

Cited by 395 publications

(439 citation statements)

References 69 publications

(101 reference statements)

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“…Vaccination or other strategies that enhance the humoral response to HIV gp120 at the CD4-binding site relative to binding of other HIV envelope epitopes may have therapeutic potential in reducing immune activation. In addition, mAbs directed against HIV are being tested currently in clinical trials to prevent HIV rebound following discontinuation of ART and are being considered in HIV prevention trials (47)(48)(49)(50). Our data demonstrate that the effects of mAb on pDC production of IFN should be considered prior to mAb selection for clinical trials because mAbs that enhance pDC production of IFN might increase immune activation.…”

Section: Discussionmentioning

confidence: 96%

HIV-antibody complexes enhance production of type I interferon by plasmacytoid dendritic cells

Veenhuis¹,

Freeman²,

Korleski³

et al. 2017

Journal of Clinical Investigation

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Section: Discussionmentioning

confidence: 96%

HIV-antibody complexes enhance production of type I interferon by plasmacytoid dendritic cells

Veenhuis¹,

Freeman²,

Korleski³

et al. 2017

Journal of Clinical Investigation

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“…Si la conception d'un vaccin capable d'induire des bNAb semble encore difficile, des immunothérapies passives, réalisées par injection d'anticorps recombinant, sont en cours d'essai clinique aux États-Unis. Ainsi, l'injection du bNAb 3BNC117 ou du VRC01, qui se fixent tous les deux sur le CD4 binding site, permet de diminuer la charge virale de 10 à 100 fois pendant 28 jours chez des patients infectés [7,8]. Le mécanisme d'action in vivo de ces anticorps reste mal compris.…”

Section: Les Fonctions Effectrices Des Immunoglobulinesunclassified

“…La plupart de ces anticorps inhibent la transmission du virus de cellule à cellule [12]. Un test révélateur de l'activation de la voie initiée par le récepteur CD16, qui est la voie de signalisation de l'ADCC dans les cellules NK, a été essais cliniques des bNAb (3BNC117 et VRC01) ne montrent pas de diminution spectaculaire de la charge en ADN viral, un marqueur de la taille du réservoir, lorsque ces anticorps sont utilisés en monothéra-pie [7,8]. Figure 2B).…”

Section: La Destruction Des Cellules Infectées Par Les Anticorps à Launclassified

Des anticorps qui détruisent les cellules infectées par le VIH-1

Bruel

Mouquet

2016

Med Sci (Paris)

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“…The breadth and potency of NIH45-46 were increased through a G54W mutation (NIH45-46 G54W ), where the tryptophan targets the Phe-43 cavity of the CD4-binding site on gp120 (11). Importantly, these highly potent broadly neutralizing antibodies (bNAbs) can protect from HIV-1 challenge and reduce viral loads in infected humanized mice and rhesus macaques and in HIV-infected individuals (12)(13)(14)(15)(16)(17).…”

mentioning

confidence: 99%

CD4-Induced Antibodies Promote Association of the HIV-1 Envelope Glycoprotein with CD4-Binding Site Antibodies

Gardner

Fellinger

Prasad

et al. 2016

J Virol

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The HIV-1 envelope glycoprotein (Env) is a trimer of gp120/gp41 heterodimers that mediates viral entry. Env binds cellular CD4, an association which stabilizes a conformation favorable to its subsequent association with a coreceptor, typically CCR5 or CXCR4. The CD4-and coreceptor-binding sites serve as epitopes for two classes of HIV-1-neutralizing antibodies: CD4-binding site (CD4bs) and CD4-induced (CD4i) antibodies, respectively. Here we observed that, at a fixed total concentration, mixtures of the CD4i antibodies (E51 or 412d) and the CD4bs antibody VRC01 neutralized the HIV-1 isolates 89.6, ADA, SG3, and SA32 more efficiently than either antibody alone. We found that E51, and to a lesser extent 412d and 17b, promoted association of four CD4bs antibodies to the Env trimer but not to monomeric gp120. We further demonstrated that the binding of the sulfotyrosine-binding pocket by CCR5mim2-Ig was sufficient for promoting CD4bs antibody binding to Env. Interestingly, the relationship is not reciprocal: CD4bs antibodies were not as efficient as CD4-Ig at promoting E51 or 412d binding to Env trimer. Consistent with these observations, CD4-Ig, but none of the CD4bs antibodies tested, substantially increased HIV-1 infection of a CD4-negative, CCR5-positive cell line. We conclude that the ability of CD4i antibodies to promote VRC01 association with Env trimers accounts for the increase potency of VRC01 and CD4i antibody mixtures. Our data further suggest that potent CD4bs antibodies avoid inducing Env conformations that bind CD4i antibodies or CCR5. IMPORTANCEPotent HIV-1-neutralizing antibodies can prevent viral transmission and suppress an ongoing infection. Here we show that CD4-induced (CD4i) antibodies, which recognize the conserved coreceptor-binding site of the HIV-1 envelope glycoprotein (Env), can increase the association of Env with potent broadly neutralizing antibodies that recognize the CD4-binding site (CD4bs antibodies). We further show that, unlike soluble forms of CD4, CD4bs antibodies poorly induce envelope glycoprotein conformations that efficiently bind CCR5. This study provides insight into the properties of potent CD4bs antibodies and suggests that, under some conditions, CD4i antibodies can improve their potency. These observations may be helpful to the development of vaccines designed to elicit specific antibody classes. Human immunodeficiency virus type 1 (HIV-1) uses its envelope glycoprotein (Env) to gain entry into host cells. Env is synthesized as precursor gp160 proteins which assemble as trimers before they are cleaved into gp120 and gp41 subunits (1). The gp120 subunit binds the primary HIV-1 receptor, CD4 (2), which then induces tertiary and quaternary conformational changes in Env that promote association with a coreceptor, usually CCR5 or CXCR4 (3, 4). The CD4-and coreceptor-binding sites are the two most conserved regions of gp120 (5, 6). Two classes of antibodies (Abs) with epitopes corresponding to each of these regions, have been defined: CD4-binding site (CD4bs) antib...

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Virologic effects of broadly neutralizing antibody VRC01 administration during chronic HIV-1 infection

Cited by 395 publications

References 69 publications

HIV-antibody complexes enhance production of type I interferon by plasmacytoid dendritic cells

HIV-antibody complexes enhance production of type I interferon by plasmacytoid dendritic cells

Des anticorps qui détruisent les cellules infectées par le VIH-1

CD4-Induced Antibodies Promote Association of the HIV-1 Envelope Glycoprotein with CD4-Binding Site Antibodies

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