2009
DOI: 10.1128/jvi.02036-08
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Factors Associated with the Development of Cross-Reactive Neutralizing Antibodies during Human Immunodeficiency Virus Type 1 Infection

Abstract: The characterization of the cross-reactive, or heterologous, neutralizing antibody responses developed during human immunodeficiency virus type 1 (HIV-1) infection and the identification of factors associated with their generation are relevant to the development of an HIV vaccine. We report that in healthy HIV-positive, antiretroviral-naïve subjects, the breadth of plasma heterologous neutralizing antibody responses correlates with the time since infection, plasma viremia levels, and the binding avidity of ant… Show more

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Cited by 485 publications
(406 citation statements)
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“…Further supporting this point, while X5 was originally considered broadly neutralizing, it has relatively poor neutralizing breadth against various HIV-1 isolates compared to the other antibodies tested here (27) yet demonstrates good breadth as a CAR. Regardless, because BNAbs seem to be escaped by HIV-1 Env variation in their original hosts (28)(29)(30), viral variability and escape may remain a barrier to the therapeutic implementation of BNAb-based CARs.…”
Section: Discussionmentioning
confidence: 99%
“…Further supporting this point, while X5 was originally considered broadly neutralizing, it has relatively poor neutralizing breadth against various HIV-1 isolates compared to the other antibodies tested here (27) yet demonstrates good breadth as a CAR. Regardless, because BNAbs seem to be escaped by HIV-1 Env variation in their original hosts (28)(29)(30), viral variability and escape may remain a barrier to the therapeutic implementation of BNAb-based CARs.…”
Section: Discussionmentioning
confidence: 99%
“…In the current study, we built upon these recent findings and used longitudinally cloned quasispecies gp160 env genes isolated from plasma from two subjects (VC10014 and VC20013). These two subtype B-infected subjects gradually developed moderate bNAbs (33) within a few years of infection by targeting two distinct regions of Env, an epitope overlapping the CD4 binding site in VC10014 and the membrane-proximal external region (MPER) in VC20013 as noted in the accompanying article by Sather et al (51). We assessed the phylogenetic and neutralization profiles and epitope exposure of the Envs based on binding to neutralizing monoclonal antibodies (NMAbs) and used these data to select a subset of variants to design vaccine strategies in rabbits.…”
mentioning
confidence: 99%
“…Prolonged antigenic exposure is a key clinical parameter associated with the natural development of bNAbs in elite neutralizers (24,(31)(32)(33), suggesting that the dynamic interactions occurring between viral quasispecies and host B cells result in continuously changing antibody specificities in vivo (24,25) and likely contribute to the generation of bNAbs (34). In fact, multiple pathways to neutralization breadth have been shown in different subjects (9,33,(35)(36)(37)(38), whereas in some subjects, antibodies with a single specificity or a few specificities can account for much of the neutralization activity (10,29,33,(39)(40)(41)(42). Thus, further understanding of the humoral response in infected individuals who naturally develop bNAbs could guide the selection of candidate Env immunogens and the design of vaccine strategies that elicit breadth (43).…”
mentioning
confidence: 99%
“…Attempts to induce such bNAbs through vaccination have mostly been ineffective. Interestingly, in natural infection, serologic breadth develops only under conditions that seem counterintuitive to efficient B cell maturation processes, such as years of chronic immune activation, loss of CD4 T cells, high levels of exhaustion marker expression, and other phenotypic lymphocyte abnormalities (2)(3)(4)(5). In addition, high viral loads and coevolution of viral quasispecies have been implicated in the development of serologic breadth, suggesting that constant immune activation and antigen recognition may play a key role in HIV antibody maturation processes.…”
mentioning
confidence: 99%