Cross-Reactive HIV-1-Neutralizing Human Monoclonal Antibodies Identified from a Patient with 2F5-Like Antibodies

Zhu, Zhongyu; Qin, Haiyan; Chen, Weizao; Zhao, Qi; Shen, Xiaoying; Schutte, Robert J.; Wang, Yanping; Ofek, Gilad; Streaker, Emily D.; Prabakaran, Ponraj; Fouda, Genevieve G.; Liao, Hua‐Xin; Owens, James D.; Louder, Mark K.; Yang, Yongping; Klaric, Kristina-Ana; Moody, M. Anthony; Mascola, John R.; Scott, Jamie K.; Kwong, Peter D.; Montefiori, David C.; Haynes, Barton F.; Tomaras, Georgia D.; Dimitrov, Dimiter S.

doi:10.1128/jvi.05312-11

Cited by 87 publications

(92 citation statements)

References 22 publications

(27 reference statements)

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“…Different studies have suggested that antibody polyreactivity contributes to neutralization of HIV-1 (24,27,31,(55)(56)(57)(58). Several mechanisms have been proposed to explain the role of antibody polyreactivity in HIV-1 neutralization.…”

Section: F425mentioning

confidence: 99%

A Cryptic Polyreactive Antibody Recognizes Distinct Clades of HIV-1 Glycoprotein 120 by an Identical Binding Mechanism

Dimitrov

Planchais

Scheel

et al. 2014

Journal of Biological Chemistry

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Background: Polyreactive antibodies can efficiently neutralize HIV. Results: Heme induces polyreactivity of a human antibody, which recognizes distinct gp120 clades by an identical binding mechanism. Conclusion: Antigen-binding promiscuity of a polyreactive antibody allows recognition of antigen with high molecular heterogeneity. Significance: Characterization of the interaction of polyreactive antibodies with envelope proteins of HIV reveals novel strategies for control of the virus.

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Section: F425mentioning

confidence: 99%

A Cryptic Polyreactive Antibody Recognizes Distinct Clades of HIV-1 Glycoprotein 120 by an Identical Binding Mechanism

Dimitrov

Planchais

Scheel

et al. 2014

Journal of Biological Chemistry

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“…1 A) overlaps that of 4E10 (39). While the epitope for m66.6 overlaps substantially with that of 2F5, this MAb is less potent and broad, neutralizing only a subset of the 2F5-sensitive viruses (64). The heavy-chain variable domains of all four Nt Abs are highly mutated and possess an unusually long third complementaritydetermining region of the antibody heavy chain (CDR-H3).…”

mentioning

confidence: 99%

“…Roughly half of the residues within this region are hydrophobic, and the MPER plays a crucial role in the fusion of the viral and cellular membranes (43). In addition, Nt epitopes within the MPER are targeted by two well-characterized broadly Nt (bNt) monoclonal Abs (MAbs) (4E10 and 2F5) (4,15,32,67) and two MAbs (Z13e1 and m66.6) that neutralize a range of viral isolates but are not bNt, making this region a promising target for vaccine efforts (39,64).…”

mentioning

confidence: 99%

Neutralizing Epitopes in the Membrane-Proximal External Region of HIV-1 gp41 Are Influenced by the Transmembrane Domain and the Plasma Membrane

Montero

Gulzar

Klaric

et al. 2012

J Virol

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“…The antigens specifically reacted with 2F5, 4E10 and a serum against the E1 domain and were immunogenic in rats generating antibodies targeting an epitope overlapping with the 2F5 epitope; however, they did not prevent HIV-1 infection in a TZM-bl based neutralisation assay. The antigens comprised the HIV-1 MPER-derived E2 domain because the corresponding bnAb antibodies are characterised by strong somatic mutations which could benefit from prolonged antigen delivery by replicating vectors [67]. Additionally, some Bet hybrids contained the FPPR derived E1 domain and the E2 domain linked by a loop to stabilise a MPER conformation that increases 2F5 binding [56,53,57,54].…”

Section: Discussionmentioning

confidence: 99%

Immunisation with foamy virus Bet fusion proteins as novel strategy for HIV-1 epitope delivery

et al. 2013

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The induction of 2F5-and 4E10-like antibodies broadly neutralising HIV-1 and targeting the membrane external proximal region (MPER) of the transmembrane envelope protein gp41 would be a major advancement for the development of a preventive HIV-1 vaccine but successful attempts remain rare. Recent studies demonstrated that broadly reactive antibodies develop relatively late during infection and after intensive affinity maturation. Therefore, a prolonged antigen delivery might be beneficial to induce them. Replicating foamy viruses which are characterised by apathogenic but persistent infection could represent suitable carrier viruses for this purpose. In order to develop such a system, we modified the accessory foamy virus Bet protein to contain the MPER of gp41, or the MPER linked to the stabilising fusion peptide proximal region (FPPR) of gp41 and analysed here the antigenic and immunogenic properties of such hybrid proteins. The antigens, expressed and purified to homogeneity, were recognised by the monoclonal antibodies 2F5 and 4E10 with nanomolar affinities and induced high levels of antibodies specific for gp41 after immunisation of rats. The antisera also bound to virus particles attached to infected cells and peptide-based epitope mapping showed that they recognised the 2F5 epitope. Although no HIV-1 neutralising activity was observed, the presented data demonstrate that using the foamy virus Bet for HIV-1 epitope delivery is successfully applicable. Together with the attractive potential for sustained antigen expression after transfer to replicating virus, these results should therefore provide a first basis for the development of chimeric foamy viruses as novel HIV-1 vaccine vectors.

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Cross-Reactive HIV-1-Neutralizing Human Monoclonal Antibodies Identified from a Patient with 2F5-Like Antibodies

Cited by 87 publications

References 22 publications

A Cryptic Polyreactive Antibody Recognizes Distinct Clades of HIV-1 Glycoprotein 120 by an Identical Binding Mechanism

A Cryptic Polyreactive Antibody Recognizes Distinct Clades of HIV-1 Glycoprotein 120 by an Identical Binding Mechanism

Neutralizing Epitopes in the Membrane-Proximal External Region of HIV-1 gp41 Are Influenced by the Transmembrane Domain and the Plasma Membrane

Immunisation with foamy virus Bet fusion proteins as novel strategy for HIV-1 epitope delivery

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