Profiling the neutralizing antibody response in chronically HIV-1 CRF07_BC-infected intravenous drug users naïve to antiretroviral therapy

Hu, Xintao; Hu, Yuanyuan; Zhao, Chen; Gao, Hongmei; Greene, Kelli; Ren, Li; Ma, Liying; Ruan, Yuhua; Sarzotti‐Kelsoe, Marcella; Montefiori, David C.; Hong, Kui; Shao, Yiming

doi:10.1038/srep46308

Cited by 6 publications

(7 citation statements)

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“…A total of 29% of plasma samples neutralized more than 80% of the tested viral strains, and 64% neutralized more than 50% in Chinese individuals infected with HIV-1 clade B 28 . The proportions of neutralizing breadths >80 and 50% were 18 and 53% in CRF07_BC-infected Chinese individuals, respectively 29 . Our group and colleagues identified a monoclonal nAb (DRVIA7) with modest neutralizing breadth from a HIV-1 B-infected Chinese donor, which was the first VRC01-like antibody isolated from Chinese donors and provided an opportunity to investigate the crucial events in the early stages of VRC01-like antibody development.…”

Section: Discussionmentioning

confidence: 98%

“…A Global Panel of reference Env clones was established by the Montefiori group at Duke University, which facilitated highly standardized assessments of neutralizing antibodies across multiple HIV-1 research platforms in different parts of the world 54 . Another separate panel containing 25 viruses was compiled by the Shao group at the Division of Research on Virology and Immunology (DRVI Panel) of China CDC, which reflected the HIV-1 epidemic in China and has been utilized in previous studies to evaluate neutralizing antibody responses 16 , 28 , 29 . Pseudoviruses HIV-1 BG505_T332N , HIV-1 BJMSM2316_N160K , and HIV-1 BJMSM2316_N332A were generated by site-directed mutagenesis based on HIV-1 BG505 and HIV-1 BJMSM2316 in this study.…”

Section: Methodsmentioning

confidence: 99%

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Identification of a novel broadly HIV-1-neutralizing antibody from a CRF01_AE-infected Chinese donor

Ren

et al. 2018

Emerging Microbes & Infections

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The isolation and characterization of monoclonal broadly neutralizing antibodies (nAbs) from natural HIV-1-infected individuals play very important roles in understanding nAb responses to HIV-1 infection and designing vaccines and therapeutics. Many broadly nAbs have been isolated from individuals infected with HIV-1 clade A, B, C, etc., but, as an important recombinant virus, the identification of broadly nAbs in CRF01_AE-infected individuals remains elusive. In this study, we used antigen-specific single B-cell sorting and monoclonal antibody expression to isolate monoclonal antibodies from a CRF01_AE-infected Chinese donor (GX2016EU04), a broad neutralizer based on neutralizing activity against a cross-clade virus panel. We identified a series of HIV-1 monoclonal cross-reactive nAbs, termed F2, H6, BF8, F4, F8, BE7, and F6. F6 could neutralize 21 of 37 tested HIV-1 Env-pseudotyped viruses (57%) with a geometric mean value of 12.15 μg/ml. Heavy and light chains of F6 were derived from IGHV4-34 and IGKV 2-28 germlines, complementarity determining region (CDR) 3 loops were composed of 18 and 9 amino acids, and somatic hypermutations (SHMs) were 16.14% and 11.83% divergent from their respective germline genes. F6 was a GP120-specific nAb and recognized the linear epitope. We identified for the first time a novel broadly HIV-1-neutralizing antibody, termed F6, from a CRF01_AE-infected donor, which could enrich the research of HIV-1 nAbs and provide useful insights for designing vaccine immunogens and antibody-based therapeutics.

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Section: Discussionmentioning

confidence: 98%

Section: Methodsmentioning

confidence: 99%

Identification of a novel broadly HIV-1-neutralizing antibody from a CRF01_AE-infected Chinese donor

Ren

et al. 2018

Emerging Microbes & Infections

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“…During the course of chronic infection, most people living with HIV-1 are eventually capable of making a polyclonal antibody response with at least moderate, but significant, breadth of coverage. Hraber et al reported that *50% of samples from chronically HIV-1-infected individuals neutralized at least 50% of 219 envelope-pseudotyped viruses, and Hu et al reported that 53% of samples from chronically HIV-1-infected individuals neutralized more than 50% of 30 envelope-pseudotyped viruses (41,43). Although immune responses in chronically infected patients cannot clear HIV-1 infections, the induction of similar responses by vaccination before an HIV-1 exposure is expected to be protective.…”

Section: Harnessing Immune Responses Toward Diverse Hiv-1 Envelope Prmentioning

confidence: 99%

Multi-Envelope HIV-1 Vaccine Development: Two Targeted Immune Pathways, One Desired Protective Outcome

Hurwitz

Bonsignori

2018

Viral Immunology

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In 2016, there were more than 30 million individuals living with HIV-1, ∼1.8 million new HIV-1 infections, and ∼1 million HIV-1-related deaths according to UNAIDS ( unaids.org ). Hence, a preventive HIV-1 vaccine remains a global priority. The variant envelopes of HIV-1 present a significant obstacle to vaccine development and the vaccine field has realized that immunization with a single HIV-1 envelope protein will not be sufficient to generate broadly neutralizing antibodies. Here we describe two nonmutually exclusive, targeted pathways with which a multi-envelope HIV-1 vaccine may generate protective immune responses against variant HIV-1. Pathways include (i) the induction of a polyclonal immune response, comprising a plethora of antibodies with subset-reactive and cross-reactive specificities, together able to neutralize diverse HIV-1 (termed Poly-nAb in this report) and (ii) the induction of one or a few monoclonal antibodies, each with a broadly neutralizing specificity (bnAb). With each pathway in mind, we describe challenges and strategies that may ultimately support HIV-1 vaccine success.

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“…The HIV-1 Env glycoprotein is highly immunogenic but, in general, the antibodies elicited by it during infection lack neutralizing breadth or potency against primary HIV-1 strains thus failing to inhibit viral replication in infected individuals 1,2 . In natural infection only 5% to 30% of adults develop broadly neutralizing antibodies (bNAbs) after several years of infection 2,3,4,5,6,7 and these bNAbs have little impact in the control of the infection due to the continuous capacity of HIV-1 to diversify and escape these antibodies 5,8,9 . However, some recombinant human bNAbs supress viral replication in HIV-1 infected individuals 10,11,12,13,14,15 , prevent human infection by some HIV-1 strains 16 , and passive immunization in animal models can protect from infection and/or disease progression (reviewed in 17 ).…”

Section: Introductionmentioning

confidence: 99%

Long-term and low-level envelope C2V3 stimulation from highly diverse virus isolates leads to frequent development of broad and elite antibody neutralization in HIV-1 infected individuals

Martin

Marcelino

Palladino

et al. 2022

Preprint

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Elicitation of potent neutralizing antibodies against genetically diverse HIV-1 isolates is important for an effective HIV-1 vaccine. Some HIV-1 infected patients produce such broadly neutralizing antibodies (bNAbs). Identification of host and viral correlates of bNAb production may help develop the next generation of HIV-1 vaccines. We carried out the first detailed characterization of the neutralizing antibody response and identify viral and host factors associated with the development of bNAbs in HIV-1 infected patients from Angola, one of the oldest, more dynamic, and diverse HIV-1 epidemics in the world. Plasma samples from 322 HIV-1 infected patients were collected in 2001, 2009 and 2014. Phylogenetic analysis of C2V3C3 envelope sequences identified a diverse array of subtypes including A1, A2, B, C, D, F1, G, H, J, untypable strains, and recombinant forms which prevailed over pure subtypes. Notably, 56% of the patients developed cross, broad, or elite neutralizing responses against a reference panel of tier 2 Env-pseudoviruses far exceeding results obtained elsewhere in the world. The frequency of elite neutralizers was higher in 2014, when patients were on ART and had low viremia, than in 2009 when patients were drug naive. In drug naive patients, broad neutralization was associated with subtype C infection, lower CD4+ T cell counts, higher age, or higher titer of C2V3C3-specific antibodies relative to patients that did not develop bNAbs. Neutralizing antibodies targeted the V3-glycan supersite in most patients but antibodies specific for the V2 apex, the CD4 binding site, the gp41 membrane-proximal external region (MPER) and unknown epitopes were also found in some patients. V3 and C3 regions were significantly less variable and less subject to positive selection in elite neutralizers compared to weak or no neutralizers suggesting an active role of bNabs directed against these regions in controlling HIV-1 replication and diversification. Hence, development of broad and elite antibody neutralization against HIV-1 requires long-term and low-level envelope V3C3 stimulation from highly diverse subtype C isolates. These results have direct implications for the design of a new generation of HIV-1 vaccines.

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Profiling the neutralizing antibody response in chronically HIV-1 CRF07_BC-infected intravenous drug users naïve to antiretroviral therapy

Cited by 6 publications

References 56 publications

Identification of a novel broadly HIV-1-neutralizing antibody from a CRF01_AE-infected Chinese donor

Identification of a novel broadly HIV-1-neutralizing antibody from a CRF01_AE-infected Chinese donor

Multi-Envelope HIV-1 Vaccine Development: Two Targeted Immune Pathways, One Desired Protective Outcome

Long-term and low-level envelope C2V3 stimulation from highly diverse virus isolates leads to frequent development of broad and elite antibody neutralization in HIV-1 infected individuals

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