Immune perturbations in HIV-1–infected individuals who make broadly neutralizing antibodies

Moody, M. Anthony; Pedroza-Pacheco, Isabela; Vandergrift, Nathan; Chui, Cecilia; Lloyd, KE; Parks, Robert; Soderberg, Kelly A.; Ogbe, Ane; Cohen, Myron S.; Hx, Liao; Gao, Feng; McMichael, Andrew J.; Montefiori, David C.; Verkoczy, Laurent; Kelsoe, Garnett; Huang, Jinghe; Shea, Patrick R.; Connors, Mark; Borrow, Persephone; Haynes, Barton F.

doi:10.1126/sciimmunol.aag0851

Cited by 108 publications

(159 citation statements)

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“…Third, the adjuvant to be used is critical, and will need to selectively drive high levels of T follicular helper cells (T fh ) and not activate or induce low levels of T regulatory cells (T reg ) in germinal centers (103, 104)(Borrow and Moody, this volume and Havenar-Daughton, Lee and Crotty, this volume).…”

Section: Resultsmentioning

confidence: 99%

“…Other bnAb types such as CD4bs antibodies are either not deleted in bone marrow or less so than gp41 antibodies, but rather antibody poly-reactivity or auto-reactivity is acquired later in bnAb B cell lineage maturation (17). Thus, for many types of bnAbs, the concept has arisen that a component of a successful vaccine for induction of bnAb B cell lineages to full neutralization breadth will be the formulation of Env vaccines in adjuvants that promote a profile of the immune system in bnAb development with high T fh and low T reg and promote repeated rounds of affinity maturation in germinal centers (103, 104). In addition, HIV-1 infection induces autoimmune manifestations in ~50% of individuals, and those HIV-1 infected individuals that make bnAbs have higher frequencies of autoantibodies than those that do not make bnAbs, indicating that bnAbs arise in the setting of HIV-1-induced loosening of immune tolerance controls (103).…”

Section: Resultsmentioning

confidence: 99%

“…Thus, for many types of bnAbs, the concept has arisen that a component of a successful vaccine for induction of bnAb B cell lineages to full neutralization breadth will be the formulation of Env vaccines in adjuvants that promote a profile of the immune system in bnAb development with high T fh and low T reg and promote repeated rounds of affinity maturation in germinal centers (103, 104). In addition, HIV-1 infection induces autoimmune manifestations in ~50% of individuals, and those HIV-1 infected individuals that make bnAbs have higher frequencies of autoantibodies than those that do not make bnAbs, indicating that bnAbs arise in the setting of HIV-1-induced loosening of immune tolerance controls (103). Thus, depending on the bnAb lineage, adjuvants or other inhibitors of immune tolerance controls may need to be utilized to achieve full bnAb maturation (Kelsoe and Haynes, this volume).…”

Section: Resultsmentioning

confidence: 99%

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

Bonsignori

Liao

Gao

et al. 2017

Immunological Reviews

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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: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

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

Bonsignori

Liao

Gao

et al. 2017

Immunological Reviews

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161

159

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“…These requirements for immunization success can be achieved by the work of antibody–virus coevo-lution and mapping (Liao et al 2013; Bon-signori et al 2016), optimization of sequential immunogensto recreate crucial events in HIV-1 infection and bnAb induction (Haynes et al 2012), and vaccine formulations that perturb immune responses to facilitate bnAb development (Gray et al 2009; Moody 2016). …”

Section: Resultsmentioning

confidence: 99%

“…Second, studies of infected individuals making bnAbs show that HIV-1 infection induces a perturbed immune state characterized by increased frequencies and levels of autoreactive antibody, increased T FH cell numbers, and decreased numbers of T regulatory cells (Treg)—a phenotype similar to the immune dysfunction observed in SLE (Gray et al 2009; Moody 2016). Combined with the autoreactive phenotypes commonly observed in bnAb KI mice (Verkoczy et al 2010; Chen et al 2013; Doyle-Cooper et al 2013; Haynes and Verkoczy 2014) and the identification of host molecules mimicked by HIV-1 Env determinants (Yang et al 2013; Liu et al 2015), these observations suggest that the reason bnAbs are not elicited by vaccines is not the inability to drive sufficient levels of V(D)J mutation but rather limitations of on-target mutation and directed affinity maturation imposed by central and peripheral immune tolerance mechanisms.…”

Section: Immune Perturbations That Occur In the Setting Of Hiv Infectionmentioning

confidence: 99%

What Are the Primary Limitations in B-Cell Affinity Maturation, and How Much Affinity Maturation Can We Drive with Vaccination?

Kelsoe

Haynes

2017

Cold Spring Harb Perspect Biol

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A key goal of HIV-1 vaccine development is the induction of broadly neutralizing antibodies (bnAbs) targeted to the vulnerable regions of the HIV envelope. BnAbs develop overtime in ∼50%of HIV-1-infected individuals. However, to date, no vaccines have induced bnAbs and few or none of these vaccine-elicited HIV-1 antibodies carry the high frequencies of V(D)J mutations characteristic of bnAbs. Do the high frequencies of mutations characteristic of naturally induced bnAbs represent a fundamental barrier to the induction of bnAbs by vaccines? Recent studies suggest that high frequencies of V(D)J mutations can be achieved by serial vaccination strategies. Rather, it appears that, in the absence of HIV-1 infection, physiologic immune tolerance controls, including a germinal center process termed affinity reversion, may limit vaccine-driven bnAb development by clonal elimination or selecting for mutations incompatible with bnAb activity.

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Strategies for induction of HIV‐1 envelope‐reactive broadly neutralizing antibodies

et al. 2021

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IntroductionA primary focus of HIV‐1 vaccine development is the activation of B cell receptors for naïve or precursor broadly neutralizing antibodies (bnAbs), followed by expansion and maturation of bnAb B cell lineage intermediates leading to highly affinity‐matured bnAbs. HIV‐1 envelope (Env) encodes epitopes for bnAbs of different specificities. Design of immunogens to induce bnAb precursors of different specificities and mature them into bnAb status is a goal for HIV‐1 vaccine development. We review vaccine strategies for bnAb lineages development and highlight the immunological barriers that these strategies must overcome to generate bnAbs.MethodsWe provide perspectives based on published research articles and reviews.DiscussionThe recent Antibody Mediated Protection (AMP) trial that tested the protective efficacy of one HIV‐1 Env bnAb specificity demonstrated that relatively high levels of long‐lasting serum titers of multiple specificities of bnAbs will be required for protection from HIV‐1 transmission. Current vaccine efforts for induction of bnAb lineages are focused on immunogens designed to expand naïve HIV‐1 bnAb precursor B cells following the recent success of vaccine‐induction of bnAb precursor B cells in macaques and humans. BnAb precursor B cells serve as templates for priming‐immunogen design. However, design of boosting immunogens for bnAb maturation requires knowledge of the optimal immunogen design and immunological environment for bnAb B cell lineage affinity maturation. BnAb lineages acquire rare genetic changes as mutations during B cell maturation. Moreover, the immunological environment that supports bnAb development during HIV‐1 infection is perturbed with an altered B cell repertoire and dysfunctional immunoregulatory controls, suggesting that in normal settings, bnAb development will be disfavoured. Thus, strategies for vaccine induction of bnAbs must circumvent immunological barriers for bnAb development that normally constrain bnAb B cell affinity maturation.ConclusionsA fully protective HIV‐1 vaccine needs to induce durable high titers of bnAbs that can be generated by a sequential set of Env immunogens for expansion and maturation of bnAb B cell lineages in a permitted immunological environment. Moreover, multiple specificities of bnAbs will be required to be sufficiently broad to prevent the escape of HIV‐1 strains during transmission.

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Immune perturbations in HIV-1–infected individuals who make broadly neutralizing antibodies

Cited by 108 publications

References 117 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

What Are the Primary Limitations in B-Cell Affinity Maturation, and How Much Affinity Maturation Can We Drive with Vaccination?

Strategies for induction of HIV‐1 envelope‐reactive broadly neutralizing antibodies

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