Polyclonal B Cell Responses to Conserved Neutralization Epitopes in a Subset of HIV-1-Infected Individuals

Tomaras, Georgia D.; Binley, James Μ.; Gray, Elin S.; Crooks, Emma T.; Osawa, Keiko; Moore, Penny L.; Tumba, Nancy; Tong, Tommy; Shen, Xiaoying; Yates, Nicole L.; Decker, Julie M.; Wibmer, Constantinos Kurt; Gao, Feng; Alam, S. Munir; Easterbrook, Philippa; Karim, Salim Safurdeen. Abdool; Kamanga, Gift; Crump, John A.; Cohen, Myron S.; Shaw, George M.; Mascola, John R.; Haynes, Barton F.; Montefiori, David C.; Morris, Lynn

doi:10.1128/jvi.05363-11

Cited by 170 publications

(181 citation statements)

References 109 publications

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“…5A and B) (228). The observation that the antiflavivirus immune response is focused on just a few specificities aligns with data from recent studies on HIV-1, in which some (255)(256)(257)(258) but not all (259)(260)(261)(262) analyses of polyclonal sera with broadly neutralizing activity suggest that just one to two specificities can recapitulate the breadth and potency of the overall serum neutralizing activity. Follow-up studies with multiple strains from each DENV serotype will be needed to explore the fine specificity of serotype-specific NAbs.…”

Section: Neutralizing Antibodies Target a Limited Number Of Specificisupporting

confidence: 81%

Deconstructing the Antiviral Neutralizing-Antibody Response: Implications for Vaccine Development and Immunity

VanBlargan

Goo

Pierson

2016

Microbiol Mol Biol Rev

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SUMMARY The antibody response plays a key role in protection against viral infections. While antiviral antibodies may reduce the viral burden via several mechanisms, the ability to directly inhibit (neutralize) infection of cells has been extensively studied. Eliciting a neutralizing-antibody response is a goal of many vaccine development programs and commonly correlates with protection from disease. Considerable insights into the mechanisms of neutralization have been gained from studies of monoclonal antibodies, yet the individual contributions and dynamics of the repertoire of circulating antibody specificities elicited by infection and vaccination are poorly understood on the functional and molecular levels. Neutralizing antibodies with the most protective functionalities may be a rare component of a polyclonal, pathogen-specific antibody response, further complicating efforts to identify the elements of a protective immune response. This review discusses advances in deconstructing polyclonal antibody responses to flavivirus infection or vaccination. Our discussions draw comparisons to HIV-1, a virus with a distinct structure and replication cycle for which the antibody response has been extensively investigated. Progress toward deconstructing and understanding the components of polyclonal antibody responses identifies new targets and challenges for vaccination strategies.

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Section: Neutralizing Antibodies Target a Limited Number Of Specificisupporting

confidence: 81%

Deconstructing the Antiviral Neutralizing-Antibody Response: Implications for Vaccine Development and Immunity

VanBlargan

Goo

Pierson

2016

Microbiol Mol Biol Rev

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“…We interpret the disproportionate frequency of short LCDR1s among CD4bs BnAbs as being indicative of a common selection process of CD4bs BnAbs that favors antibodies with shortened LCDR1s. This is the first chronically infected SLE individual with concomitant HIV-1 infection that we have been able to study, and it was striking that this individual also had robust plasma BnAb activity, given that the incidence of chronically HIV-1-infected subjects with this level of plasma neutralization breadth is only approximately 20% (49)(50)(51)(52).…”

Section: Figurementioning

confidence: 86%

An autoreactive antibody from an SLE/HIV-1 individual broadly neutralizes HIV-1

Bonsignori¹,

Wiehe²,

Grimm³

et al. 2014

J. Clin. Invest.

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Broadly HIV-1-neutralizing antibodies (BnAbs) display one or more unusual traits, including a long heavy chain complementarity-determining region 3 (HCDR3), polyreactivity, and high levels of somatic mutations. These shared characteristics suggest that BnAb development might be limited by immune tolerance controls. It has been postulated that HIV-1-infected individuals with autoimmune disease and defective immune tolerance mechanisms may produce BnAbs more readily than those without autoimmune diseases. In this study, we identified an HIV-1-infected individual with SLE who exhibited controlled viral load (<5,000 copies/ml) in the absence of controlling HLA phenotypes and developed plasma HIV-1 neutralization breadth. We collected memory B cells from this individual and isolated a BnAb, CH98, that targets the CD4 binding site (CD4bs) of HIV-1 envelope glycoprotein 120 (gp120). CH98 bound to human antigens including dsDNA, which is specifically associated with SLE. Anti-dsDNA reactivity was also present in the patient's plasma. CH98 had a mutation frequency of 25% and 15% nt somatic mutations in the heavy and light chain variable domains, respectively, a long HCDR3, and a deletion in the light chain CDR1. The occurrence of anti-dsDNA reactivity by a HIV-1 CD4bs BnAb in an individual with SLE raises the possibility that some BnAbs and SLE-associated autoantibodies arise from similar pools of B cells.

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“…Algorithms based on common patterns of neutralizing activity against panels of diverse Env strains are available, that can rapidly estimate whether a new bnAb targets a known epitope (75–79). Often times the epitope can be confirmed by testing neutralizing activity against mutant strains that contain known bnAb-specific diagnostic escape mutations (80, 81). Moreover, computational analyses of Env sequences and corresponding patterns of bnAb activity have been used to identify genetic signatures within and outside bnAb epitopes that compliment crystal structure information in guiding novel immunogen designs (82, 83) (Korber, Hraber, Wagh and Hahn, this volume).…”

Section: Neutralization Assessment Of Bnab Lineage Developmentmentioning

confidence: 99%

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

Bonsignori

Liao

Gao

et al. 2017

Immunological Reviews

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156

150

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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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Polyclonal B Cell Responses to Conserved Neutralization Epitopes in a Subset of HIV-1-Infected Individuals

Cited by 170 publications

References 109 publications

Deconstructing the Antiviral Neutralizing-Antibody Response: Implications for Vaccine Development and Immunity

Deconstructing the Antiviral Neutralizing-Antibody Response: Implications for Vaccine Development and Immunity

An autoreactive antibody from an SLE/HIV-1 individual broadly neutralizes HIV-1

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

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