Dengue type 1 viruses circulating in humans are highly infectious and poorly neutralized by human antibodies

Raut, Rajendra; Ks, Corbett; Rn, Tennekoon; Premawansa, Sunil; Wijewickrama, Ananda; Premawansa, Gayani; Mieczkowski, Piotr A.; Rückert, Claudia; Gd, Ebel; Ad, De Silva; Silva, de

doi:10.1073/pnas.1812055115

Cited by 76 publications

(108 citation statements)

References 30 publications

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“…Therefore, the detection of DENV within the biopsy tissue suggests that a persistent infection was established prior to immune suppression and that this infection did not arise from later therapeutic attempts. 29 Together, the observations from our patient and other flaviviruses suggest that virus within the host may be resistant to immune pressures and that the CNS may be an underappreciated anatomical reservoir for flaviviruses. For example, West Nile virus has been detected intermittently in urine up to 6 years postinfection in patients with previous West Nile virus encephalitis.…”

Section: Discussionmentioning

confidence: 59%

Chronic Dengue Virus Panencephalitis in a Patient with Progressive Dementia with Extrapyramidal Features

Johnson

Larman

Lee

et al. 2019

Annals of Neurology

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Objective: To determine the underlying etiology in a patient with progressive dementia with extrapyramidal signs and chronic inflammation referred to the National Institutes of Health Undiagnosed Diseases Program. Methods: Extensive investigations included metabolic profile, autoantibody panel, infectious etiologies, genetic screening, whole exome sequencing, and the phage-display assay, VirScan, for viral immune responses. An etiological diagnosis was established postmortem. Results: Using VirScan, enrichment of dengue viral antibodies was detected in cerebrospinal fluid as compared to serum. No virus was detected in serum or cerebrospinal fluid, but postmortem analysis confirmed dengue virus in the brain by immunohistochemistry, in situ hybridization, quantitative polymerase chain reaction, and sequencing. Dengue virus was also detectable by polymerase chain reaction and sequencing from brain biopsy tissue collected 33 months antemortem, confirming a chronic infection despite a robust immune response directed against the virus. Immunoprofiling and whole exome sequencing of the patient did not reveal any immunodeficiency, and sequencing of the virus demonstrated wild-type dengue virus in the central nervous system. Interpretation: Dengue virus is the most common arbovirus worldwide and represents a significant public health concern. Infections with dengue virus are usually self-limiting, and chronic dengue infections have not been previously reported. Our findings suggest that dengue virus infections may persist in the central nervous system causing a panencephalitis and should be considered in patients with progressive dementia with extrapyramidal features in endemic regions or with relevant travel history. Furthermore, this work highlights the utility of comprehensive antibody profiling assays to aid in the diagnosis of encephalitis of unknown etiology.

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Section: Discussionmentioning

confidence: 59%

Chronic Dengue Virus Panencephalitis in a Patient with Progressive Dementia with Extrapyramidal Features

Johnson

Larman

Lee

et al. 2019

Annals of Neurology

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“…However, it is noted that ZIKV RVPs are made in defined cell types (typically BHK cells), and there is evidence suggesting that some flavivirus properties, particularly maturity, can be influenced by the producing cell type (whether live virus or RVP) (47).…”

Section: Discussionmentioning

confidence: 99%

“…Maturation of flaviviruses occurs by the cleavage of the prM protein to M (9), but this is generally incomplete, with virus maturity (whether live virus or RVP) (Cherrier 2009; ref for ZIKV) being influenced by the producing cell type (Dejninarattisai et al, 2015). In addition, patient-derived DENV showed higher levels of maturity compared with the same virus following passage in cells (47,48). The maturation state of flaviviruses is thought to be important for infectivity and for neutralization by sera in clinical studies.…”

Section: Generation Of Zikv Rvps With Distinct Maturation Statesmentioning

confidence: 99%

Antigenicity, stability, and reproducibility of Zika reporter virus particles for long-term applications

Whitbeck

Thomas

Kadash-Edmondson

et al. 2020

Preprint

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The development of vaccines against flaviviruses, including Zika virus (ZIKV) and dengue virus (DENV), continues to be a major challenge, hindered by the lack of efficient and reliable methods for screening neutralizing activity of sera or antibodies. To address this need, we previously developed a plasmid-based, replication-incompetent DENV reporter virus particle (RVP) production system as an efficient and safe alternative to the Plaque Reduction Neutralization Test (PRNT). As part of the response to the 2015-2016 ZIKV outbreak, we recently developed pseudoinfectious ZIKV RVPs by modifying our DENV RVP system. The use of ZIKV RVPs as critical reagents in human clinical trials requires their further validation using stability and reproducibility metrics for large-scale applications. In the current study, we validated ZIKV RVPs using infectivity, neutralization, and enhancement assays with monoclonal antibodies (MAbs) and human ZIKV-positive patient serum. ZIKV RVPs are antigenically identical to live virus based on binding ELISA and neutralization results and are nonreplicating based on the results of plaque formation assays. We demonstrate reproducible neutralization titer data (NT50 values) across different RVP production lots, volumes, time frames, and laboratories. We also show RVP stability across experimentally relevant time intervals and temperatures. Our results demonstrate that ZIKV RVPs provide a safe, rapid, and reproducible reagent for large-scale, long-term studies of neutralizing antibodies and sera, which can facilitate large-scale screening and epidemiological studies to help expedite ZIKV vaccine development.

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“…However, the suboptimal efficacy and safety profile of a recently licensed DENV vaccine has been partly attributed to its inability to generate a balanced neutralizing antibody response to all four serotypes (Hadinegoro et al, 2015). Additionally, there may be important antigenic differences between circulating and lab-adapted strains (Lim et al, 2019;Raut et al, 2019), as well as among strains even within a given serotype (Bell, Katzelnick, & Bedford, 2019;Katzelnick et al, 2015). Antigenic mismatch between vaccine and circulating strains impacted vaccine efficacy (Juraska et al, 2018), highlighting the importance of rational selection of vaccine components.…”

Section: Introductionmentioning

confidence: 99%

“…J9 and J8 also potently neutralized contemporary DENV1-4 isolates with IC50 values < 50 ng/ml ( Figure S3). Additionally, in contrast to C4 and the crossreactive DII fusion loop-specific mouse mAb E60 (Goo, VanBlargan, Dowd, Diamond, & Pierson, 2017;Nelson et al, 2008;Oliphant et al, 2006), but similar to EDE bNAbs (Dejnirattisai et al, 2015), J9 and J8 potently neutralized DENV regardless of virion maturation state ( Figure S4), which can indirectly modulate epitope exposure (Cherrier et al, 2009;Goo et al, 2019;Nelson et al, 2008) and has been shown to be distinct among circulating versus labadapted strains (Raut et al, 2019). We also tested the ability of mAbs to mediate neutralization after virus attachment to cells, which is characteristic of many potently neutralizing antibodies against flaviviruses (Goo et al, 2019;Nybakken et al, 2005;Sukupolvi-Petty et al, 2010;Vogt et al, 2009;Xu et al, 2017).…”

Section: Introductionmentioning

confidence: 99%

Functional characterization and lineage analysis of broadly neutralizing human antibodies against dengue virus identified by single B cell transcriptomics

Durham

Agrawal

Waltari

et al. 2019

Preprint

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Eliciting broadly neutralizing antibodies (bNAbs) against the four dengue virus serotypes (DENV1-4) that are spreading into new territories is an important goal of vaccine design. To delineate bNAb targets, we characterized 28 monoclonal antibodies belonging to expanded and hypermutated clonal families identified by transcriptomic analysis of single plasmablasts from DENV-infected individuals. Among these, we identified two somatically related bNAbs that potently neutralized DENV1-4. Mutagenesis studies revealed that the major recognition determinants of these bNAbs are in E protein domain I, distinct from the only known class of human bNAbs against flaviviruses with a well-defined epitope. B cell repertoire analysis from acute-phase peripheral blood suggested a memory origin and divergent somatic hypermutation pathways for these bNAbs, and a limited number of mutations was sufficient for neutralizing activity. Our study suggests multiple B cell evolutionary pathways leading to DENV bNAbs targeting a novel epitope that can be exploited for vaccine design. E monomeric subunits within the dimer. A subset of these E dimer epitope (EDE)-specific bNAbs potently neutralize not only DENV1-4, but also ZIKV, owing to the high conservation of the EDE, which overlaps the prM binding site on E ( Barba-Spaeth et al., 2016;Dejnirattisai et al., 2015;Rouvinski et al., 2015). The exciting discovery of the EDE class of bNAbs highlights the potential for an epitope-focused flavivirus vaccine strategy.As multiple specificities are likely required to provide maximum coverage of diverse circulating viral variants (Bell et al., 2019;Doria-Rose et al., 2012;Goo, Jalalian-Lechak, Richardson, & Overbaugh, 2012;Katzelnick et al., 2015; Keeffe et al., 2018; Kong et al., 2015), in this study, we aimed to define novel sites on the flavivirus E protein that can be targeted by bNAbs. By characterizing 28 monoclonal antibodies from the plasmablasts of two DENV-infected individuals, we identified J8 and J9, clonally related bNAbs that neutralized DENV1-4 in the low picomolar range. The major recognition determinants for J8 and J9 were in E protein DI, distinct from previously characterized bNAbs. Analysis of the corresponding B cell repertoire revealed divergent evolution of J8 and J9, suggesting multiple evolutionary pathways to generate bNAbs within this lineage. Our work identifies both viral and host determinants of the development of DENV bNAbs that can guide immunogen design and evaluation. Results Identification of cross-reactive neutralizing antibodies from clonally expanded plasmablasts of DENV-infected individualsWe previously profiled the single-cell transcriptomics of peripheral blood mononuclear cells (PBMCs) from six dengue patients and four healthy individuals (Zanini et al., 2018). In two DENV-infected patients (013 and 020), we identified 15 clonal families comprising a total of 38 unique paired heavy (VH) and light (VL) chain IgG1 plasmablast sequences, some of which were hypermutated (1.67% to 10.77% for VH, 0.67% to 7.22% for...

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Dengue type 1 viruses circulating in humans are highly infectious and poorly neutralized by human antibodies

Cited by 76 publications

References 30 publications

Chronic Dengue Virus Panencephalitis in a Patient with Progressive Dementia with Extrapyramidal Features

Chronic Dengue Virus Panencephalitis in a Patient with Progressive Dementia with Extrapyramidal Features

Antigenicity, stability, and reproducibility of Zika reporter virus particles for long-term applications

Functional characterization and lineage analysis of broadly neutralizing human antibodies against dengue virus identified by single B cell transcriptomics

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