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

Durham, Natasha D.; Agrawal, Aditi; Waltari, Eric; Croote, Derek; Zanini, Fabio; Davidson, Edgar; Fouch, Mallorie E.; Smith, Olivia; Carabajal, Esteban; Pak, John E.; Doranz, Benjamin J.; Robinson, Makeda; Sanz, A.; Albornoz, Ludwig L; Rosso, Fernando; Einav, Shirit; Quake, Stephen R.; McCutcheon, Krista; Goo, Leslie

doi:10.1101/790642

Cited by 3 publications

(6 citation statements)

References 99 publications

(102 reference statements)

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“…To rule out a mouse antibody-specific artifact, we next performed the above ADE assays using a broadly reactive human monoclonal anti-DENV IgG antibody, J9 [ 75 ]. In these assays, TBC1D24 KO ( Figure 2A ) and SV2B KO ( Figure 2B ) each resulted in a ∼50% reduction in AUC compared to WT cells.…”

Section: Resultsmentioning

confidence: 99%

“…TBC1D24 and SV2B are required for efficient ADE but not direct infection. ( A-B ) (Left) Representative dose-response ADE curves for K562 ( A ) TBC1D24 KO clone ( B ) SV2B KO clone, and genetically trans -complemented K562 KO cells infected with DENV2-GFP in the presence of serially diluted human anti-DENV IgG monoclonal antibody J9 [ 75 ]. In each experiment, K562 WT cell pool and a FcgRIIa KO clone was included as a control.…”

Section: Resultsmentioning

confidence: 99%

See 1 more Smart Citation

Functional genomics screens reveal a role for TBC1D24 and SV2B in antibody-dependent enhancement of dengue virus infection

Belmont,

Contreras,

Cartwright-Acar

et al. 2024

Preprint

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Dengue virus (DENV) can hijack non-neutralizing IgG antibodies to facilitate its uptake into target cells expressing Fc gamma receptors (FcgR) - a process known as antibody-dependent enhancement (ADE) of infection. Beyond a requirement for FcgR, host dependency factors for this non-canonical infection route remain unknown. To identify cellular factors exclusively required for ADE, here, we performed CRISPR knockout screens in an in vitro system permissive to infection only in the presence of IgG antibodies. Validating our approach, a top hit was FcgRIIa, which facilitates binding and internalization of IgG-bound DENV but is not required for canonical infection. Additionally, we identified host factors with no previously described role in DENV infection, including TBC1D24 and SV2B, both of which have known functions in regulated secretion. Using genetic knockout and trans-complemented cells, we validated a functional requirement for these host factors in ADE assays performed with monoclonal antibodies and polyclonal sera in multiple cell lines and using all four DENV serotypes. We show that knockout of TBC1D24 or SV2B impaired binding of IgG-DENV complexes to cells without affecting FcgRIIa expression levels. Thus, we identify cellular factors beyond FcgR that are required for ADE of DENV infection. Our findings represent a first step towards advancing fundamental knowledge behind the biology of ADE that can ultimately be exploited to inform vaccination and therapeutic approaches.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Functional genomics screens reveal a role for TBC1D24 and SV2B in antibody-dependent enhancement of dengue virus infection

Belmont,

Contreras,

Cartwright-Acar

et al. 2024

Preprint

Self Cite

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show abstract

“…Previous efforts to characterize antigenicity of flavivirus surface proteins have not been able to distinguish between functionally required residues for neutralization versus binding [23][24][25][26]28 . Other efforts, such as phage display platforms to perform alanine scanning of dengue virus and small scale site-directed mutagenesis could only identify linear antibody epitopes, and only provide limited information on a few domains of E 16,17,38 . In contrast, our approach comprehensively measures the effect of all single amino acid mutations on neutralization by antibodies with complex quaternary epitopes.…”

Section: Discussionmentioning

confidence: 99%

The effect of single mutations in Zika virus envelope on escape from broadly neutralizing antibodies

Kikawa,

Cartwright-Acar,

Stuart

et al. 2023

Preprint

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Zika virus and dengue virus are co-circulating flaviviruses with a widespread endemic range. Eliciting broad and potent neutralizing antibodies is an attractive goal for developing a vaccine to simultaneously protect against these viruses. However, the capacity of viral mutations to confer escape from broadly neutralizing antibodies remains undescribed, due in part to limited throughput and scope of traditional approaches. Here, we use deep mutational scanning to map how all possible single amino acid mutations in Zika virus envelope protein affect neutralization by antibodies of varying breadth and potency. While all antibodies selected viral escape mutations, the mutations selected by broadly neutralizing antibodies conferred less escape relative to those selected by narrow, virus-specific antibodies. Surprisingly, even for broadly neutralizing antibodies with similar binding footprints, different single mutations led to escape, indicating distinct functional requirements for neutralization not captured by existing structures. Additionally, the antigenic effects of mutations selected by broadly neutralizing antibodies were conserved across divergent, albeit related, flaviviruses. Our approach identifies residues critical for antibody neutralization, thus comprehensively defining the as-yet-unknown functional epitopes of antibodies with clinical potential.ImportanceThe wide endemic range of mosquito-vectored flaviviruses – such as Zika virus and dengue virus serotypes 1-4 – places hundreds of millions of people at risk of infection every year. Despite this, there are no widely available vaccines, and treatment of severe cases is limited to supportive care. An avenue towards development of more widely applicable vaccines and targeted therapies is the characterization of monoclonal antibodies that broadly neutralize all these viruses. Here, we measure how single amino acid mutations in viral envelope protein affect neutralizing antibodies with both broad and narrow specificities. We find that broadly neutralizing antibodies with potential as vaccine prototypes or biological therapeutics are quantifiably more difficult to escape than narrow, virus-specific neutralizing antibodies.

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“…Previous efforts to characterize antigenicity of flavivirus surface proteins have not been able to distinguish between functionally required residues for neutralization versus binding ( 23 – 26 , 28 ). Other efforts, such as phage display platforms to perform alanine scanning of dengue virus and small scale site-directed mutagenesis, could only identify linear antibody epitopes and only provide limited information on a few domains of E ( 16 , 17 , 39 ). In contrast, our approach comprehensively measures the effect of all single amino acid mutations on neutralization by antibodies with complex quaternary epitopes.…”

Section: Discussionmentioning

confidence: 99%

“…Thus, there is immense interest in both developing vaccines that elicit broad and potent neutralizing antibody responses, as well as isolating and leveraging broadly neutralizing antibodies as biological therapeutics. Toward this end, investigations have examined human antibody repertoires and isolated a select few antibodies that can broadly and potently neutralize Zika virus and all serotypes of dengue virus ( 16 – 20 ). These antibodies all target envelope (E) protein, which is the major antigenic target in both Zika virus and dengue virus ( 21 , 22 ).…”

Section: Introductionmentioning

confidence: 99%

The effect of single mutations in Zika virus envelope on escape from broadly neutralizing antibodies

Kikawa,

Cartwright-Acar,

Stuart

et al. 2023

J Virol

Self Cite

View full text Add to dashboard Cite

Zika virus and dengue virus are co-circulating flaviviruses with a widespread endemic range. Eliciting broad and potent neutralizing antibodies is an attractive goal for developing a vaccine to simultaneously protect against these viruses. However, the capacity of viral mutations to confer escape from broadly neutralizing antibodies remains undescribed, due in part to limited throughput and scope of traditional approaches. Here, we use deep mutational scanning to map how all possible single amino acid mutations in Zika virus envelope protein affect neutralization by antibodies of varying breadth and potency. While all antibodies selected viral escape mutations, the mutations selected by broadly neutralizing antibodies conferred less escape relative to those selected by narrow, virus-specific antibodies. Surprisingly, even for broadly neutralizing antibodies with similar binding footprints, different single mutations led to escape, indicating distinct functional requirements for neutralization not captured by existing structures. Additionally, the antigenic effects of mutations selected by broadly neutralizing antibodies were conserved across divergent, albeit related, flaviviruses. Our approach identifies residues critical for antibody neutralization, thus comprehensively defining the as-yet-unknown functional epitopes of antibodies with clinical potential. IMPORTANCE The wide endemic range of mosquito-vectored flaviviruses—such as Zika virus and dengue virus serotypes 1–4—places hundreds of millions of people at risk of infection every year. Despite this, there are no widely available vaccines, and treatment of severe cases is limited to supportive care. An avenue toward development of more widely applicable vaccines and targeted therapies is the characterization of monoclonal antibodies that broadly neutralize all these viruses. Here, we measure how single amino acid mutations in viral envelope protein affect neutralizing antibodies with both broad and narrow specificities. We find that broadly neutralizing antibodies with potential as vaccine prototypes or biological therapeutics are quantifiably more difficult to escape than narrow, virus-specific neutralizing antibodies.

show abstract

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

Cited by 3 publications

References 99 publications

Functional genomics screens reveal a role for TBC1D24 and SV2B in antibody-dependent enhancement of dengue virus infection

Functional genomics screens reveal a role for TBC1D24 and SV2B in antibody-dependent enhancement of dengue virus infection

The effect of single mutations in Zika virus envelope on escape from broadly neutralizing antibodies

The effect of single mutations in Zika virus envelope on escape from broadly neutralizing antibodies

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