Broad neutralization coverage of HIV by multiple highly potent antibodies

Walker, Laura M.; Huber, Michael; Doores, Katie J.; Falkowska, Emilia; Pejchal, Robert; Julien, Jean-Philippe; Wang, Shengkai; Ramos, Alejandra; Chan-Hui, Po-Ying; Moyle, Matthew; Mitcham, Jennifer L.; Hammond, Phillip W.; Olsen, Ole; Phung, Pham; Fling, Steven P.; Wong, Chi‐Huey; Phogat, Sanjay; Wrin, Terri; Simek, Melissa; Investigators, Protocol G. Principal; Koff, Wayne C.; Wilson, Ian A.; Burton, Dennis R.; Poignard, Pascal

doi:10.1038/nature10373

Cited by 1,369 publications

(1,891 citation statements)

References 34 publications

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“…The V3-glycan PCDN, BF520-derived and DH270 bnAb lineages share some common traits: 1) differently from previously described V3-gylcan bnAbs (23, 25), their evolution did not involve insertion/deletion (indel) events, demonstrating that indels are not a universal requirement for the V3-glycan bnAb class to acquire neutralization breadth; 2) neutralization breadth was acquired with relatively modest levels of somatic hypermutation that can be achieved through vaccination (57, 60, 61), and 3) the UCA of the V3-glycan lineages did not neutralize or bind autologous TF suggesting the hypothesis that V3-glycan bnAb lineages may arise in response to altered forms of the Env protein.…”

Section: Antibody-virus Co-evolutionmentioning

confidence: 92%

Antibody‐virus co‐evolution in HIV infection: paths for HIV vaccine development

Bonsignori

Liao

Gao

et al. 2017

Immunological Reviews

155

143

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Summary Induction of HIV-1 broadly neutralizing antibodies (bnAbs) to date has only been observed in the setting of HIV-1 infection, and then only years after HIV transmission. Thus, the concept has emerged that one path to induction of bnAbs is to define the viral and immunologic events that occur during HIV-1 infection, and then to mimic those events with a vaccine formulation. This concept has led to efforts to map both virus and antibody events that occur from the time of HIV-1 transmission to development of bnAbs. This work has revealed that a virus-antibody “arms race” occurs in which a HIV-1 transmitted/founder (TF) Env induces autologous neutralizing antibodies that can not only neutralize the TF virus but also can select virus escape mutants that in turn select affinity-matured neutralizing antibodies. From these studies has come a picture of bnAb development that has led to new insights in host-pathogen interactions and, as well, led to insight into immunologic mechanisms of control of bnAb development. Here we review the progress to date in elucidating bnAb B cell lineages in HIV-1 infection, discuss new research leading to understanding the immunologic mechanisms of bnAb induction, and address issues relevant to the use of this information for the design of new HIV-1 sequential envelope vaccine candidates.

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Section: Antibody-virus Co-evolutionmentioning

confidence: 92%

Antibody‐virus co‐evolution in HIV infection: paths for HIV vaccine development

Bonsignori

Liao

Gao

et al. 2017

Immunological Reviews

155

143

View full text Add to dashboard Cite

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“…The glycan site at residue 160 is typically critical for these bnAbs and a decrease in neutralization is seen when additional glycan sites are removed from the V1, V2, and V3 loops in a viral isolate‐dependent manner 66. With the isolation of additional N160‐dependent apex bnAbs, by our group and others,22, 42, 51, 67 this class can be divided into four groups typified by the prototypes PG9, CH01, PGT145, and CAP256.VRC26.09 (CAP256.09) 68. All four prototypes bind N160 and basic residues in the lysine‐rich strand C of the V2 loop, but the exact residues required for each epitope vary, with a lysine at position 169 the most commonly shared feature 68.…”

Section: Specificity Of Hiv Bnabsmentioning

confidence: 95%

“…Subsequently, advances in the production of soluble near‐native stabilized Env trimers46 have allowed better selection of Env‐specific B cells, excluding those which bind regions not exposed on the infectious viral spike. Using this method, we isolated PGDM140028 from the same donor that previously yielded the PGT141–145 family of bnAbs via the B‐cell culturing approach 22. Furthermore, stabilized BG505 SOSIP.664 trimers have been used as baits to isolate two bnAbs which occupy overlapping epitopes at the gp120‐gp41 interface and also contact the fusion peptide, ACS20247 and VRC34 48.…”

Section: Identification Of Hiv Bnabsmentioning

confidence: 99%

“…By comparing structural information generated for different families within this class, it was shown that the N332/GDIR epitope is accessed from a variety of angles by the different bnAbs, which use diverse binding modes, leading to its definition as a supersite of vulnerability 71. Furthermore, in contrast to some other bnAb classes, these high‐mannose patch bnAbs use a variety of V, D, and J germline genes and do not appear to share particular genetic traits required for binding this epitope 22, 71. Thus, it would be difficult to use an NGS approach to identify bnAbs from new donors even if the serum neutralization was clearly N332 dependent.…”

Section: Specificity Of Hiv Bnabsmentioning

confidence: 99%

“…High‐throughput neutralization assays were a major factor in changing that situation. The ability to analyze mAb and serum activity against large panels of viruses was demonstrated20 and subsequently used to evaluate large numbers of HIV‐infected donors in the International AIDS Vaccine Initiative (IAVI) Protocol G and C studies to identify those with exceptionally potent and broad sera,8 map the specificities underlying these responses,7, 21 and then isolate bnAbs from these individuals 22, 23, 24, 25, 26, 27, 28. Independently, the standardization of the TZM‐bl neutralization assay and the definition of neutralization sensitivity tiers29, 30, 31 allowed much more rigorous serum analysis.…”

Section: Introductionmentioning

confidence: 99%

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Identification and specificity of broadly neutralizing antibodies against HIV

McCoy

Burton

2017

Immunological Reviews

Self Cite

204

189

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SummaryBeginning in 2009, studies of the humoral responses of HIV‐positive individuals have led to the identification of scores, if not hundreds, of antibodies that are both broadly reactive and potently neutralizing. This development has provided renewed impetus toward an HIV vaccine and led directly to the development of novel immunogens. Advances in identification of donors with the most potent and broad anti‐HIV serum neutralizing responses were crucial in this effort. Equally, development of methods for the rapid generation of human antibodies from these donors was pivotal. Primarily these methods comprise single B‐cell culture coupled to high‐throughput neutralization screening and flow cytometry‐based sorting of single B cells using HIV envelope protein baits. In this review, the advantages and disadvantages of these methodologies are discussed in the context of the specificities targeted by individual antibodies and the need for further improvements to evaluate HIV vaccine candidates.

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Monoclonal Antibodies

Zola

Engel

2015

Encyclopedia of Life Sciences

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Antibodies bind to target molecules strongly and specifically and are therefore useful reagents in research, diagnosis and therapy. Antibodies taken from the blood of immunised animals are a mixture of different immunoglobulins produced by many B cells, and are known as polyclonal antibodies. In contrast, monoclonal antibodies are antibodies with a unique specificity, generally made by cells containing a particular immunoglobulin gene set derived from a single cell or a clone of B cells. Monoclonal antibodies can be produced in cell culture and are therefore more reproducible from batch to batch than polyclonal antibodies. Most of the monoclonal antibodies currently used were generated from mice using the hybridoma technology. However, recently powerful alternative technologies have been developed for the generation of monoclonal antibodies, especially fully human antibodies. These methods are based on the cloning and sequencing of the immunoglobulin genes from antigen‐specific B cells followed by the generation of recombinant antibodies. Monoclonal antibodies have become essential reagents in many research and diagnostic applications, and are increasingly used in therapy, generating a multibillion dollar industry. Key Concepts Antibodies form part of the vertebrate immune response, binding with high affinity and specificity to target molecules (antigens). Antibodies are able to neutralise and remove antigens and modulate biological functions. Antibodies that bind to target molecules can be made by injecting an animal with antigens, from immune individuals or synthetic libraries. One B cells makes just one antibody with a unique specificity, but from the blood, we get a mixture of the antibodies produced by many B cells (polyclonal antibodies). A monoclonal antibody is an antibody, which is obtained by expanding and immortalising a single clone of B‐cells with a defined specificity. Monoclonal antibodies provide specific reagents for almost any molecular structure. Monoclonal antibodies can be used to identify, quantify, isolate or remove the target molecule in complex biological mixtures or in tissues. Monoclonal antibodies can be injected into patients for the treatment of a wide range of diseases including infections, cancer, cardiovascular diseases and autoimmune diseases. Advances in molecular biological technologies make it possible to modify monoclonal antibodies to achieve enhanced therapeutic effects with minimal side effects.

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Broad neutralization coverage of HIV by multiple highly potent antibodies

Cited by 1,369 publications

References 34 publications

Antibody‐virus co‐evolution in HIV infection: paths for HIV vaccine development

Antibody‐virus co‐evolution in HIV infection: paths for HIV vaccine development

Identification and specificity of broadly neutralizing antibodies against HIV

Monoclonal Antibodies

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