A cocktail of protective antibodies subverts the dense glycan shield of Lassa virus

Li, Hao-Yang; Buck, Tierra; Zandonatti, Michelle; Yin, Jieyun; Moon-Walker, Alex; Fang, Jingru; Koval, Anatoliy; Heinrich, Megan L.; Rowland, Megan M.; Avalos, Ruben Diaz; Schendel, Sharon L.; Parekh, Diptiben; Zyla, Dawid; Enriquez, Adrian; Harkins, Stephanie; Sullivan, Brian M.; Smith, Victoria I.; Chukwudozie, Onyeka S; Watanabe, Reika; Robinson, James E.; Garry, Robert F.; Branco, Luis M.; Hastie, Kathryn M.; Saphire, Erica Ollmann

doi:10.1126/scitranslmed.abq0991

Cited by 18 publications

(34 citation statements)

References 59 publications

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“…In addition to the approved and previously authorized mAbs and those directed against SARS-CoV-2, many other mAbs have been or are under development against existing and emerging diseases (see [58][59][60][61] for some examples). Historically, therapeutic mAbs were derived from immunized mice or rats and engineered as chimeric or humanized mAbs to reduce the immunogenicity due the "foreignness" of rodent mAbs in humans.…”

Section: Monoclonal Antibodiesmentioning

confidence: 99%

Uses and Challenges of Antiviral Polyclonal and Monoclonal Antibody Therapies

Struble¹,

Rawson²,

Stantchev³

et al. 2023

Preprint

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Viral diseases represent a major public health concern and an ever-present risk for developing into a future pandemic. Antiviral antibody therapeutics, either alone or in combination with other therapies, have emerged as valuable preventative and treatment options, including during a global emergency. Here we will discuss polyclonal and monoclonal antiviral antibody therapies, focusing on the unique biochemical and physiological properties that make them well suited as therapeutic agents. We will describe the methods of antibody characterization and potency assessment throughout development, highlighting similarities and differences between polyclonal and monoclonal products as appropriate. In addition, we will consider the benefits and challenges of antiviral antibodies when used in combination with other antibodies or other types of antiviral therapeutics. Lastly, we will discuss novel approaches to the characterization and development of antiviral antibodies and identify areas that would benefit from additional research.

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Section: Monoclonal Antibodiesmentioning

confidence: 99%

Uses and Challenges of Antiviral Polyclonal and Monoclonal Antibody Therapies

Struble¹,

Rawson²,

Stantchev³

et al. 2023

Preprint

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show abstract

“…This highly potent broadly neutralizing antibody (bNAb) directly blocks matriglycan binding and has been shown to require the native cleavage site to engage with GPC. 29 Therefore, to generate a trimeric GPC immunogen that presents all currently known bNAb epitopes, we reverted the RRRR site of GPCysR4 to the native RRLL sequence.…”

Section: Development and Characterization Of Recombinant Lasv Gpc Tri...mentioning

confidence: 99%

“…27,28 Since then, methods have been described to stabilize the trimeric conformation of prefusion GPC in the absence of a trimer-stabilizing mAb. [29][30][31] We previously demonstrated that prefusion GPC trimers are stabilized by genetic fusion to the trimeric scaffold I53-50A. 30,31 These fusion proteins, known as GPC-I53-50A, have not only proven to be a useful reagent for characterizing and isolating GPC-specific antibodies but also were able to induce NAb responses in rabbits.…”

Section: Introductionmentioning

confidence: 99%

“…39 Nevertheless, numerous potent NAbs have been isolated from convalescent individuals and the mechanism of action for several of these NAbs has been elucidated. 15,[27][28][29]31,40,41 Cocktails of isolated NAbs have shown great promise as therapeutics in animal models. For example, Arevirumab-3, a cocktail of NAbs 8.9F, 37.2D and 12.1F, shows protection in non-human primates after LASV challenge.…”

Section: Introductionmentioning

confidence: 99%

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Defining bottlenecks and opportunities for Lassa virus neutralization by structural profiling of vaccine-induced polyclonal antibody responses

Brouwer,

Perrett,

Beaumont

et al. 2023

Preprint

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SummaryLassa fever continues to be a major public health burden in endemic countries in West Africa, yet effective therapies or vaccines are lacking. The isolation of potent and protective neutralizing antibodies against the Lassa virus glycoprotein complex (GPC) justifies the development of vaccines that can elicit strong neutralizing antibody responses. However, Lassa vaccines candidates have generally been unsuccessful in doing so and the associated antibody responses to these vaccines remain poorly characterized. Here, we establish an electron-microscopy based epitope mapping pipeline that enables high-resolution structural characterization of polyclonal antibodies to GPC. By applying this method to rabbits vaccinated with a recombinant GPC vaccine and a GPC-derived virus-like particle, we reveal determinants of neutralization which involve epitopes of the GPC-C, GPC-A, and GP1-A competition clusters. Furthermore, by identifying previously undescribed immunogenic off-target epitopes, we expose challenges that recombinant GPC vaccines face. By enabling detailed polyclonal antibody characterization, our work ushers in a next generation of more rational Lassa vaccine design.

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“…28 Some of these antibodies are being developed as antibody cocktails and there is evidence that they can protect from lethal Lassa virus infection. [29][30][31][32] In addition, vaccines that elicit antibodies against GPC are also being developed. [33][34][35][36][37] However, the high variability of GPC (up to ~8% amino-acid divergence among lineages) raises the specter of antibody and vaccine escape, a problem that has been observed for other viruses-including most recently SARS-CoV-2.…”

Section: Introductionmentioning

confidence: 99%

Deep mutational scanning reveals functional constraints and antigenic variability of Lassa virus glycoprotein complex

Carr,

Crawford,

Murphy

et al. 2024

Preprint

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Lassa virus is estimated to cause thousands of human deaths per year, primarily due to spillovers from its natural host,Mastomysrodents. Efforts to create vaccines and antibody therapeutics must account for the evolutionary variability of Lassa virus’s glycoprotein complex (GPC), which mediates viral entry into cells and is the target of neutralizing antibodies. To map the evolutionary space accessible to GPC, we use pseudovirus deep mutational scanning to measure how nearly all GPC amino-acid mutations affect cell entry and antibody neutralization. Our experiments define functional constraints throughout GPC. We quantify how GPC mutations affect neutralization by a panel of monoclonal antibodies and show that all antibodies are escaped by mutations that exist among natural Lassa virus lineages. Overall, our work describes a biosafety-level-2 method to elucidate the mutational space accessible to GPC and shows how prospective characterization of antigenic variation could aid design of therapeutics and vaccines.

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A cocktail of protective antibodies subverts the dense glycan shield of Lassa virus

Cited by 18 publications

References 59 publications

Uses and Challenges of Antiviral Polyclonal and Monoclonal Antibody Therapies

Uses and Challenges of Antiviral Polyclonal and Monoclonal Antibody Therapies

Defining bottlenecks and opportunities for Lassa virus neutralization by structural profiling of vaccine-induced polyclonal antibody responses

Deep mutational scanning reveals functional constraints and antigenic variability of Lassa virus glycoprotein complex

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