20 results on '"Barbara Guarino"'
Search Results
2. Therapeutic Administration of Broadly Neutralizing FI6 Antibody Reveals Lack of Interaction Between Human IgG1 and Pig Fc Receptors
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Sophie B. Morgan, Barbara Holzer, Johanneke D. Hemmink, Francisco J. Salguero, John C. Schwartz, Gloria Agatic, Elisabetta Cameroni, Barbara Guarino, Emily Porter, Pramila Rijal, Alain Townsend, Bryan Charleston, Davide Corti, and Elma Tchilian
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influenza ,anti-stem antibody ,pig ,Fc receptor ,FI6 ,enhanced disease ,Immunologic diseases. Allergy ,RC581-607 - Abstract
Influenza virus infection is a significant global health threat. Because of the lack of cross-protective universal vaccines, short time window during which antivirals are effective and drug resistance, new therapeutic anti-influenza strategies are required. Broadly, cross-protective antibodies that target conserved sites in the hemagglutinin (HA) stem region have been proposed as therapeutic agents. FI6 is the first proven such monoclonal antibody to bind to H1–H16 and is protective in mice and ferrets. Multiple studies have shown that Fc-dependent mechanisms are essential for FI6 in vivo efficacy. Here, we show that therapeutic administration of FI6 either intravenously or by aerosol to pigs did not reduce viral load in nasal swabs or broncho-alveolar lavage, but aerosol delivery of FI6 reduced gross pathology significantly. We demonstrate that pig Fc receptors do not bind human IgG1 and that FI6 did not mediate antibody-dependent cytotoxicity (ADCC) with pig PBMC, confirming that ADCC is an important mechanism of protection by anti-stem antibodies in vivo. Enhanced respiratory disease, which has been associated with pigs with cross-reactive non-neutralizing anti-HA antibodies, did not occur after FI6 administration. Our results also show that in vitro neutralizing antibody responses are not a robust correlate of protection for the control of influenza infection and pathology in a natural host model.
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- 2018
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3. A pan-influenza antibody inhibiting neuraminidase via receptor mimicry
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Corey Momont, Ha V. Dang, Fabrizia Zatta, Kevin Hauser, Caihong Wang, Julia di Iulio, Andrea Minola, Nadine Czudnochowski, Anna De Marco, Kaitlin Branch, David Donermeyer, Siddhant Vyas, Alex Chen, Elena Ferri, Barbara Guarino, Abigail E. Powell, Roberto Spreafico, Samantha S. Yim, Dale R. Balce, Istvan Bartha, Marcel Meury, Tristan I. Croll, David M. Belnap, Michael A. Schmid, William Timothy Schaiff, Jessica L. Miller, Elisabetta Cameroni, Amalio Telenti, Herbert W. Virgin, Laura E. Rosen, Lisa A. Purcell, Antonio Lanzavecchia, Gyorgy Snell, Davide Corti, Matteo Samuele Pizzuto, di Iulio, Julia [0000-0001-9343-127X], Chen, Alex [0000-0003-2620-5066], Spreafico, Roberto [0000-0001-8282-7658], Yim, Samantha S [0009-0007-8567-3501], Belnap, David M [0000-0002-0619-7487], Schmid, Michael A [0000-0002-1137-9322], Telenti, Amalio [0000-0001-6290-7677], Rosen, Laura E [0000-0002-8030-0219], Purcell, Lisa A [0000-0002-9565-2030], Snell, Gyorgy [0000-0003-1475-659X], Corti, Davide [0000-0002-5797-1364], Pizzuto, Matteo Samuele [0000-0001-5776-654X], and Apollo - University of Cambridge Repository
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Multidisciplinary ,Influenza A Virus, H3N2 Subtype ,Molecular Mimicry ,Antibodies, Monoclonal ,Hemagglutinins, Viral ,Neuraminidase ,Antibodies, Viral ,Arginine ,Mice ,Influenza B virus ,Orthomyxoviridae Infections ,Antibody Specificity ,Influenza A virus ,Influenza Vaccines ,Catalytic Domain ,Influenza, Human ,Sialic Acids ,Animals ,Humans ,Seasons - Abstract
Rapidly evolving influenza A viruses (IAVs) and influenza B viruses (IBVs) are major causes of recurrent lower respiratory tract infections. Current influenza vaccines elicit antibodies predominantly to the highly variable head region of haemagglutinin and their effectiveness is limited by viral drift1 and suboptimal immune responses2. Here we describe a neuraminidase-targeting monoclonal antibody, FNI9, that potently inhibits the enzymatic activity of all group 1 and group 2 IAVs, as well as Victoria/2/87-like, Yamagata/16/88-like and ancestral IBVs. FNI9 broadly neutralizes seasonal IAVs and IBVs, including the immune-evading H3N2 strains bearing an N-glycan at position 245, and shows synergistic activity when combined with anti-haemagglutinin stem-directed antibodies. Structural analysis reveals that D107 in the FNI9 heavy chain complementarity-determinant region 3 mimics the interaction of the sialic acid carboxyl group with the three highly conserved arginine residues (R118, R292 and R371) of the neuraminidase catalytic site. FNI9 demonstrates potent prophylactic activity against lethal IAV and IBV infections in mice. The unprecedented breadth and potency of the FNI9 monoclonal antibody supports its development for the prevention of influenza illness by seasonal and pandemic viruses.
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- 2023
4. Therapeutic and vaccine-induced cross-reactive antibodies with effector function against emerging Omicron variants
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Amin Addetia, Luca Piccoli, James Brett Case, Young-Jun Park, Martina Beltramello, Barbara Guarino, Ha Dang, Dora Pinto, Suzanne M. Scheaffer, Kaitlin Sprouse, Jessica Bassi, Chiara Silacci-Fregni, Francesco Muoio, Marco Dini, Lucia Vincenzetti, Rima Acosta, Daisy Johnson, Sambhavi Subramanian, Christian Saliba, Martina Giurdanella, Gloria Lombardo, Giada Leoni, Katja Culap, Carley McAlister, Anushka Rajesh, Exequiel Dellota, Jiayi Zhou, Nisar Farhat, Dana Bohan, Julia Noack, Florian A. Lempp, Elisabetta Cameroni, Bradley Whitener, Olivier Giannini, Alessandro Ceschi, Paolo Ferrari, Alessandra Franzetti-Pellanda, Maira Biggiogero, Christian Garzoni, Stephanie Zappi, Luca Bernasconi, Min Jeong Kim, Gretja Schnell, Nadine Czudnochowski, Nicholas Franko, Jennifer K. Logue, Courtney Yoshiyama, Cameron Stewart, Helen Chu, Michael A. Schmid, Lisa A. Purcell, Gyorgy Snell, Antonio Lanzavecchia, Michael S. Diamond, Davide Corti, and David Veesler
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Article - Abstract
Currently circulating SARS-CoV-2 variants acquired convergent mutations at receptor-binding domain (RBD) hot spots1. Their impact on viral infection, transmission, and efficacy of vaccines and therapeutics remains poorly understood. Here, we demonstrate that recently emerged BQ.1.1. and XBB.1 variants bind ACE2 with high affinity and promote membrane fusion more efficiently than earlier Omicron variants. Structures of the BQ.1.1 and XBB.1 RBDs bound to human ACE2 and S309 Fab (sotrovimab parent) explain the altered ACE2 recognition and preserved antibody binding through conformational selection. We show that sotrovimab binds avidly to all Omicron variants, promotes Fc-dependent effector functions and protects mice challenged with BQ.1.1, the variant displaying the greatest loss of neutralization. Moreover, in several donors vaccine-elicited plasma antibodies cross-react with and trigger effector functions against Omicron variants despite reduced neutralizing activity. Cross-reactive RBD-directed human memory B cells remained dominant even after two exposures to Omicron spikes, underscoring persistent immune imprinting. Our findings suggest that this previously overlooked class of cross-reactive antibodies, exemplified by S309, may contribute to protection against disease caused by emerging variants through elicitation of effector functions.
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- 2023
5. Imprinted antibody responses against SARS-CoV-2 Omicron sublineages
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Young-Jun Park, Dora Pinto, Alexandra C. Walls, Zhuoming Liu, Anna De Marco, Fabio Benigni, Fabrizia Zatta, Chiara Silacci-Fregni, Jessica Bassi, Kaitlin R. Sprouse, Amin Addetia, John E. Bowen, Cameron Stewart, Martina Giurdanella, Christian Saliba, Barbara Guarino, Michael A. Schmid, Nicholas M. Franko, Jennifer K. Logue, Ha V. Dang, Kevin Hauser, Julia di Iulio, William Rivera, Gretja Schnell, Anushka Rajesh, Jiayi Zhou, Nisar Farhat, Hannah Kaiser, Martin Montiel-Ruiz, Julia Noack, Florian A. Lempp, Javier Janer, Rana Abdelnabi, Piet Maes, Paolo Ferrari, Alessandro Ceschi, Olivier Giannini, Guilherme Dias de Melo, Lauriane Kergoat, Hervé Bourhy, Johan Neyts, Leah Soriaga, Lisa A. Purcell, Gyorgy Snell, Sean P. J. Whelan, Antonio Lanzavecchia, Herbert W. Virgin, Luca Piccoli, Helen Y. Chu, Matteo Samuele Pizzuto, Davide Corti, David Veesler, University of Washington [Seattle], Humabs BioMed SA, Washington University School of Medicine [Saint Louis, MO], Vir Biotechnology Inc [San Francisco], Catholic University of Leuven - Katholieke Universiteit Leuven (KU Leuven), Università della Svizzera italiana = University of Italian Switzerland (USI), Lugano Regional Hospital [Lugano], University of New South Wales [Sydney] (UNSW), University hospital of Zurich [Zurich], Bellinzona Regional Hospital [Bellinzona], Lyssavirus, épidémiologie et neuropathologie - Lyssavirus Epidemiology and Neuropathology, Institut Pasteur [Paris] (IP)-Université Paris Cité (UPCité), University of Texas Southwestern Medical Center [Dallas], and This study was supported by the National Institute of Allergy and Infectious Diseases (DP1AI158186 and HHSN272201700059C to D.V.), a Pew Biomedical Scholars Award (D.V.), an Investigators in the Pathogenesis of Infectious Disease Awards from the Burroughs Wellcome Fund (D.V.), Fast Grants (D.V.), the University of Washington Arnold and Mabel Beckman cryoEM center and the National Institute of Health grant S10OD032290 (to D.V.). S.P.J.W. supported be NIH grant AI163019. D.V. is an Investigator of the Howard Hughes Medical Institute. O.G. is funded by the Swiss Kidney Foundation.
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Multidisciplinary ,SARS-CoV-2 ,COVID-19 ,Antibodies, Viral ,Antibodies, Neutralizing ,Article ,Memory B Cells ,Neutralization Tests ,Antibody Formation ,Spike Glycoprotein, Coronavirus ,Humans ,[SDV.IMM]Life Sciences [q-bio]/Immunology ,Immunologic Memory ,[SDV.MHEP]Life Sciences [q-bio]/Human health and pathology ,Immune Evasion - Abstract
Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) Omicron sublineages carry distinct spike mutations resulting in escape from antibodies induced by previous infection or vaccination. We show that hybrid immunity or vaccine boosters elicit plasma-neutralizing antibodies against Omicron BA.1, BA.2, BA.2.12.1, and BA.4/5, and that breakthrough infections, but not vaccination alone, induce neutralizing antibodies in the nasal mucosa. Consistent with immunological imprinting, most antibodies derived from memory B cells or plasma cells of Omicron breakthrough cases cross-react with the Wuhan-Hu-1, BA.1, BA.2, and BA.4/5 receptor-binding domains, whereas Omicron primary infections elicit B cells of narrow specificity up to 6 months after infection. Although most clinical antibodies have reduced neutralization of Omicron, we identified an ultrapotent pan-variant-neutralizing antibody that is a strong candidate for clinical development. ispartof: SCIENCE vol:378 issue:6620 pages:619-+ ispartof: location:United States status: published
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- 2022
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6. Antibody-mediated broad sarbecovirus neutralization through ACE2 molecular mimicry
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Barbara Guarino, Young-Jun Park, Tyler N. Starr, Herbert W. Virgin, Florian A. Lempp, Matteo Samuele Pizzuto, Anshu Joshi, Sean P. J. Whelan, Gyorgy Snell, Alexandra C. Walls, Zhuoming Liu, Jesse D. Bloom, Johan Neyts, Julia Noack, Fabrizia Zatta, Davide Corti, Martina Giurdanella, Samantha K Zepeda, Dora Pinto, Rana Abdelnabi, Fabio Benigni, John E. Bowen, Kaitlin S Sprouse, David Veesler, Anna De Marco, and Shi-Yan Caroline Foo
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Models, Molecular ,Protein Conformation ,medicine.drug_class ,viruses ,Mutant ,Antibody Affinity ,Cross Reactions ,Antibodies, Viral ,medicine.disease_cause ,Monoclonal antibody ,Article ,Epitope ,Neutralization ,Betacoronavirus ,Epitopes ,Protein Domains ,Immunity ,medicine ,Animals ,Humans ,Binding site ,Immune Evasion ,Multidisciplinary ,Mesocricetus ,biology ,SARS-CoV-2 ,Cryoelectron Microscopy ,Molecular Mimicry ,Antibodies, Monoclonal ,COVID-19 ,Virology ,Molecular mimicry ,Mutation ,Spike Glycoprotein, Coronavirus ,biology.protein ,Angiotensin-Converting Enzyme 2 ,Antibody ,Broadly Neutralizing Antibodies ,Receptors, Coronavirus - Abstract
Understanding broadly neutralizing sarbecovirus antibody responses is key to developing countermeasures against severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) variants and future zoonotic sarbecoviruses. We describe the isolation and characterization of a human monoclonal antibody, designated S2K146, that broadly neutralizes viruses belonging to SARS-CoV– and SARS-CoV-2–related sarbecovirus clades, which use angiotensin-converting enzyme 2 (ACE2) as an entry receptor. Structural and functional studies show that most of the virus residues that directly bind S2K146 are also involved in binding to ACE2. This allows the antibody to potently inhibit receptor attachment. S2K146 protects against SARS-CoV-2 Beta variant challenge in hamsters, and viral passaging experiments reveal a high barrier for emergence of escape mutants, making it a good candidate for clinical development. The conserved ACE2-binding residues present a site of vulnerability that might be leveraged for developing vaccines eliciting broad sarbecovirus immunity.
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- 2022
7. Broad betacoronavirus neutralization by a stem helix-specific human antibody
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Megan Smithey, Rana Abdelnabi, John E. Bowen, M. Alejandra Tortorici, Hannah Kaiser, Saiful Islam, Katja Culap, Nicole Sprugasci, Dora Pinto, Herbert W. Virgin, Pietro E. Cippà, Gyorgy Snell, Antonio Lanzavecchia, Olivier Giannini, Michael P. Housley, Nadine Czudnochowski, Fabio Benigni, Barbara Guarino, Amalio Telenti, Johan Neyts, David I. Hong, Roberta Marzi, Antonino Cassotta, Samuele Ceruti, Eneida Vetti, Stefano Jaconi, Julia di Iulio, David Veesler, Laura E. Rosen, Agostino Riva, Chiara Silacci-Fregni, Elisabetta Cameroni, Florian A. Lempp, Alessandro Ceschi, Martina Beltramello, Colin Havenar-Daughton, Jessica Bassi, Lotte Coelmont, Siro Bianchi, Luca Piccoli, Julia Noack, Jun Siong Low, Istvan Bartha, Caroline S. Foo, Maximilian M. Sauer, Davide Corti, Josipa Jerak, Paolo Ferrari, Christian Garzoni, Matteo Samuele Pizzuto, Alexandra C. Walls, and Federica Sallusto
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Protein Conformation, alpha-Helical ,Somatic cell ,viruses ,PROTEIN ,ACE2 ,medicine.disease_cause ,Membrane Fusion ,Neutralization ,Jurkat Cells ,0302 clinical medicine ,DOMAIN ,NANOPARTICLE VACCINES ,Cricetinae ,INFECTION ,Lung ,Coronavirus ,chemistry.chemical_classification ,0303 health sciences ,Multidisciplinary ,biology ,virus diseases ,Antibodies, Monoclonal ,Viral Load ,Multidisciplinary Sciences ,Spike Glycoprotein, Coronavirus ,Science & Technology - Other Topics ,CORONAVIRUS SPIKE GLYCOPROTEIN ,Antibody ,medicine.drug_class ,SARS-COV-2 ,Cross Reactions ,Monoclonal antibody ,Peptide Mapping ,03 medical and health sciences ,Betacoronavirus ,Immunoglobulin Fab Fragments ,Neutralization Tests ,medicine ,Animals ,Humans ,030304 developmental biology ,Science & Technology ,IDENTIFICATION ,MUTATIONS ,SARS-CoV-2 ,Lipid bilayer fusion ,Convalescence ,Viral Vaccines ,Virus Internalization ,biology.organism_classification ,Virology ,Antibodies, Neutralizing ,Immunoglobulin Fc Fragments ,chemistry ,biology.protein ,Glycoprotein ,030217 neurology & neurosurgery ,RESPONSES - Abstract
The spillovers of betacoronaviruses in humans and the emergence of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) variants highlight the need for broad coronavirus countermeasures. We describe five monoclonal antibodies (mAbs) cross-reacting with the stem helix of multiple betacoronavirus spike glycoproteins isolated from COVID-19 convalescent individuals. Using structural and functional studies, we show that the mAb with the greatest breadth (S2P6) neutralizes pseudotyped viruses from three different subgenera through the inhibition of membrane fusion, and we delineate the molecular basis for its cross-reactivity. S2P6 reduces viral burden in hamsters challenged with SARS-CoV-2 through viral neutralization and Fc-mediated effector functions. Stem helix antibodies are rare, oftentimes of narrow specificity, and can acquire neutralization breadth through somatic mutations. These data provide a framework for structure-guided design of pan-betacoronavirus vaccines eliciting broad protection. ispartof: SCIENCE vol:373 issue:6559 pages:1109-1115 ispartof: location:United States status: published
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- 2021
8. Broad sarbecovirus neutralization by a human monoclonal antibody
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Jesse D. Bloom, Fabio Benigni, Anna De Marco, Fabrizia Zatta, Laura E. Rosen, Stefano Jaconi, Istvan Bartha, Tyler N. Starr, Michael P. Housley, Elisabetta Cameroni, Julia di Iulio, Gyorgy Snell, Rana Abdelnabi, Davide Corti, Chiara Silacci Fregni, Jiayi Zhou, Katja Culap, Exequiel Dellota, Herbert W. Virgin, Nicole Sprugasci, John E. Bowen, Isabella Giacchetto-Sasselli, M. Alejandra Tortorici, David Veesler, Nadine Czudnochowski, Dora Pinto, Shi Yan Caroline Foo, Martina Beltramello, Colin Havenar-Daughton, Christian Saliba, Zhuoming Liu, Matteo Samuele Pizzuto, Samantha K Zepeda, Hannah Kaiser, Amalio Telenti, Johan Neyts, Roberta Marzi, Martin Montiel-Ruiz, Alexandra C. Walls, Michael A. Schmid, Z. Wang, Sean P. J. Whelan, Barbara Guarino, Eneida Vetti, Florian A. Lempp, and Amin Addetia
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education.field_of_study ,Multidisciplinary ,Zoonotic Infection ,biology ,medicine.drug_class ,Population ,biology.organism_classification ,Monoclonal antibody ,Virology ,Epitope ,Antigenic drift ,Article ,Antigen ,medicine ,biology.protein ,Antibody ,education ,Mesocricetus - Abstract
The recent emergence of SARS-CoV-2 variants of concern1-10 and the recurrent spillovers of coronaviruses11,12 into the human population highlight the need for broadly neutralizing antibodies that are not affected by the ongoing antigenic drift and that can prevent or treat future zoonotic infections. Here we describe a human monoclonal antibody designated S2X259, which recognizes a highly conserved cryptic epitope of the receptor-binding domain and cross-reacts with spikes from all clades of sarbecovirus. S2X259 broadly neutralizes spike-mediated cell entry of SARS-CoV-2, including variants of concern (B.1.1.7, B.1.351, P.1, and B.1.427/B.1.429), as well as a wide spectrum of human and potentially zoonotic sarbecoviruses through inhibition of angiotensin-converting enzyme 2 (ACE2) binding to the receptor-binding domain. Furthermore, deep-mutational scanning and in vitro escape selection experiments demonstrate that S2X259 possesses an escape profile that is limited to a single substitution, G504D. We show that prophylactic and therapeutic administration of S2X259 protects Syrian hamsters (Mesocricetus auratus) against challenge with the prototypic SARS-CoV-2 and the B.1.351 variant of concern, which suggests that this monoclonal antibody is a promising candidate for the prevention and treatment of emergent variants and zoonotic infections. Our data reveal a key antigenic site that is targeted by broadly neutralizing antibodies and will guide the design of vaccines that are effective against all sarbecoviruses.
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- 2021
9. A human antibody that broadly neutralizes betacoronaviruses protects against SARS-CoV-2 by blocking the fusion machinery
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Alessandro Ceschi, Herbert W. Virgin, Agostino Riva, Istvan Bartha, David K. Hong, Roberta Marzi, Antonino Cassotta, Elisabetta Cameroni, Saiful Islam, Katja Culap, Laura E. Rosen, Nicole Sprugasci, Julia di Iulio, Antonio Lanzavecchia, Julia Noack, Nadine Czudnochowski, Caroline S. Foo, Barbara Guarino, Samuele Ceruti, M. Alejandra Tortorici, Lotte Coelmont, David Veesler, Eneida Vetti, Jun Siong Low, Martina Beltramello, Colin Havenar-Daughton, Rana Abdelnabi, Dora Pinto, Florian A. Lempp, Luca Piccoli, Federica Sallusto, Stefano Jaconi, Maximilian M. Sauer, Gyorgy Snell, Jessica Bassi, Matteo Samuele Pizzuto, Davide Corti, Chiara Silacci-Fregni, John E. Bowen, Amalio Telenti, Michael P. Housley, Paolo Ferrari, Alexandra C. Walls, Hanna Kaiser, Siro Bianchi, Fabio Benigni, Josipa Jerak, Meghan Smithey, and Johan Neyts
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chemistry.chemical_classification ,medicine.drug_class ,viruses ,virus diseases ,Lipid bilayer fusion ,Biology ,medicine.disease_cause ,Monoclonal antibody ,Virology ,Epitope ,Neutralization ,chemistry ,Viral entry ,medicine ,biology.protein ,Antibody ,Glycoprotein ,Coronavirus - Abstract
The repeated spillovers of {beta}-coronaviruses in humans along with the rapid emergence of SARS-CoV-2 escape variants highlight the need to develop broad coronavirus therapeutics and vaccines. Five monoclonal antibodies (mAbs) were isolated from COVID-19 convalescent individuals and found to cross-react with multiple {beta}-coronavirus spike (S) glycoproteins by targeting the stem helix. One of these mAbs, S2P6, cross-reacts with more than twenty human and animal {beta}-coronavirus S glycoproteins and broadly neutralizes SARS-CoV-2 and pseudotyped viruses from the sarbecovirus, merbecovirus and embecovirus subgenera. Structural and functional studies delineate the molecular basis of S2P6 cross-reactivity and broad neutralization and indicate that this mAb blocks viral entry by inhibiting membrane fusion. S2P6 protects hamsters challenged with SARS-CoV-2 (including the B.1.351 variant of concern) through direct viral neutralization and Fc-mediated effector functions. Serological and B cell repertoire analyses indicate that antibodies targeting the stem helix are found in some convalescent donors and vaccinees but are predominantly of narrow specificity. Germline reversion of the identified cross-reactive mAbs revealed that their unmutated ancestors are specific for the endemic OC43 or HKU1 viruses and acquired enhanced affinity and breadth through somatic mutations. These data demonstrate that conserved epitopes in the coronavirus fusion machinery can be targeted by protective antibodies and provide a framework for structure-guided design of pan-{beta}-coronavirus vaccines eliciting broad protection.
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- 2021
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10. Structural basis for broad sarbecovirus neutralization by a human monoclonal antibody
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Tyler N. Starr, Michael P. Housley, Michael A. Schmid, Roberta Marzi, Martin Montiel-Ruiz, Katja Culap, Hanna Kaiser, Matteo Samuele Pizzuto, Nicole Sprugasci, Barbara Guarino, David Veesler, Fabio Benigni, Johan Neyts, Nadine Czudnochowski, Eneida Vetti, Exequiel Dellota, Martina Beltramello, Colin Havenar-Daughton, M. Alejandra Tortorici, Isabella Giacchetto-Sasselli, Florian A. Lempp, Caroline S. Foo, Dora Pinto, Anna De Marco, Gyorgy Snell, Julia di Iulio, Stefano Jaconi, Rana Abdelnabi, Z. Wang, Jiayi Zhou, Chiara Silacci Fregni, Amalio Telenti, Fabrizia Zatta, Jesse D. Bloom, Laura E. Rosen, Davide Corti, Herbert W. Virgin, Alexandra C. Walls, Christian Saliba, Samantha K Zepeda, Sean P. J. Whelan, Amin Addetia, John E. Bowen, Istvan Bartha, Elisabetta Cameroni, and Zhuoming Liu
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medicine.drug_class ,Population ,Cross Reactions ,Monoclonal antibody ,Antibodies, Viral ,Viral Zoonoses ,Epitope ,Antigenic drift ,Neutralization ,Article ,Antigen ,Neutralization Tests ,medicine ,Animals ,Humans ,education ,Immune Evasion ,education.field_of_study ,biology ,Zoonotic Infection ,Mesocricetus ,SARS-CoV-2 ,Antibodies, Monoclonal ,COVID-19 ,Virology ,Disease Models, Animal ,Mutation ,biology.protein ,Female ,Antibody ,Broadly Neutralizing Antibodies - Abstract
The recent emergence of SARS-CoV-2 variants of concern (VOC) and the recurrent spillovers of coronaviruses in the human population highlight the need for broadly neutralizing antibodies that are not affected by the ongoing antigenic drift and that can prevent or treat future zoonotic infections. Here, we describe a human monoclonal antibody (mAb), designated S2×259, recognizing a highly conserved cryptic receptor-binding domain (RBD) epitope and cross-reacting with spikes from all sarbecovirus clades. S2×259 broadly neutralizes spike-mediated entry of SARS-CoV-2 including the B.1.1.7, B.1.351, P.1 and B.1.427/B.1.429 VOC, as well as a wide spectrum of human and zoonotic sarbecoviruses through inhibition of ACE2 binding to the RBD. Furthermore, deep-mutational scanning and in vitro escape selection experiments demonstrate that S2×259 possesses a remarkably high barrier to the emergence of resistance mutants. We show that prophylactic administration of S2×259 protects Syrian hamsters against challenges with the prototypic SARS-CoV-2 and the B.1.351 variant, suggesting this mAb is a promising candidate for the prevention and treatment of emergent VOC and zoonotic infections. Our data unveil a key antigenic site targeted by broadly-neutralizing antibodies and will guide the design of pan-sarbecovirus vaccines.
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- 2021
11. The dual function monoclonal antibodies VIR-7831 and VIR-7832 demonstrate potent in vitro and in vivo activity against SARS-CoV-2
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Andrea L. Cathcart, Colin Havenar-Daughton, Florian A. Lempp, Daphne Ma, Michael A. Schmid, Maria L. Agostini, Barbara Guarino, Julia Di iulio, Laura E. Rosen, Heather Tucker, Joshua Dillen, Sambhavi Subramanian, Barbara Sloan, Siro Bianchi, Dora Pinto, Christian Saliba, Katja Culap, Jason A Wojcechowskyj, Julia Noack, Jiayi Zhou, Hannah Kaiser, Sooyoung Lee, Nisar Farhat, Arthur Chase, Martin Montiel-Ruiz, Exequiel Dellota, Arnold Park, Roberto Spreafico, Anna Sahakyan, Elvin J. Lauron, Nadine Czudnochowski, Elisabetta Cameroni, Sarah Ledoux, Yoshihiro Kawaoka, Adam Werts, Christophe Colas, Leah Soriaga, Amalio Telenti, Lisa A. Purcell, Seungmin Hwang, Gyorgy Snell, Herbert W. Virgin, Davide Corti, and Christy M. Hebner
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medicine.drug_class ,biochemical phenomena, metabolism, and nutrition ,Biology ,Monoclonal antibody ,Virology ,Fragment crystallizable region ,Virus ,Epitope ,In vitro ,In vivo ,medicine ,biology.protein ,bacteria ,Antibody ,Viral load - Abstract
VIR-7831 and VIR-7832 are dual action monoclonal antibodies (mAbs) targeting the spike glycoprotein of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2). VIR-7831 and VIR-7832 were derived from a parent antibody (S309) isolated from memory B cells of a 2003 severe acute respiratory syndrome coronavirus (SARS-CoV) survivor. Both mAbs contain an “LS” mutation in the Fc region to prolong serum half-life and potentially enhance distribution to the respiratory mucosa. In addition, VIR-7832 encodes an Fc GAALIE mutation that has been shown previously to evoke CD8+ T-cells in the context of an in vivo viral respiratory infection. VIR-7831 and VIR-7832 potently neutralize wild-type and variant authentic virus in vitro as well as variant pseudotyped viruses. In addition, they retain activity against monoclonal antibody resistance mutations conferring reduced susceptibility to currently authorized mAbs. The VIR-7831/VIR-7832 epitope does not overlap with mutational sites in current variants of concern and continues to be highly conserved among circulating sequences consistent with the high barrier to resistance observed in vitro. Furthermore, both mAbs can recruit effector mechanisms in vitro that may contribute to clinical efficacy via elimination of infected host cells. In vitro studies with these mAbs demonstrated no enhancement of infection. In a Syrian Golden hamster proof-of concept wildtype SARS-CoV-2 infection model, animals treated with VIR-7831 had less weight loss, and significantly decreased total viral load and infectious virus levels in the lung compared to a control mAb. Taken together, these data indicate that VIR-7831 and VIR-7832 are promising new agents in the fight against COVID-19.
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- 2021
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12. N-terminal domain antigenic mapping reveals a site of vulnerability for SARS-CoV-2
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David Veesler, Matthew McCallum, Herbert W. Virgin, Shi Yan Caroline Foo, Davide Corti, John E. Bowen, Julia di Iulio, M. Alejandra Tortorici, Agostino Riva, Chiara Silacci Fregni, Rana Abdelnabi, Louis Marie Bloyet, Johan Neyts, Anna De Marco, Amalio Telenti, Zhuoming Liu, Jiayi Zhou, Matteo Samuele Pizzuto, Gyorgy Snell, Paul W. Rothlauf, Fabrizia Zatta, Alexander Chen, Elisabetta Cameroni, Samantha K Zepeda, Fabio Benigni, Martina Beltramello, Dora Pinto, Alexandra C. Walls, Laura E. Rosen, Siro Bianchi, Sean P. J. Whelan, Martin Montiel-Ruiz, Barbara Guarino, and Florian A. Lempp
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Models, Molecular ,PROTEIN ,ACE2 ,CORONAVIRUS ,medicine.disease_cause ,Epitope ,0302 clinical medicine ,Cricetinae ,CRYO-EM STRUCTURE ,Neutralizing antibody ,Antigens, Viral ,Coronavirus ,chemistry.chemical_classification ,0303 health sciences ,biology ,Antibodies, Monoclonal ,Entry into host ,Monoclonal ,RNA, Viral ,SPIKE GLYCOPROTEIN ,Antibody ,Life Sciences & Biomedicine ,Biochemistry & Molecular Biology ,Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) ,Protein domain ,VALIDATION ,Article ,General Biochemistry, Genetics and Molecular Biology ,STRUCTURAL DEFINITION ,03 medical and health sciences ,Protein Domains ,Antigen ,Neutralization Tests ,NEUTRALIZING ANTIBODY ,medicine ,Animals ,030304 developmental biology ,Science & Technology ,RECEPTOR-BINDING DOMAIN ,SARS-CoV-2 ,MUTATIONS ,COVID-19 ,Genetic Variation ,Cell Biology ,Antibodies, Neutralizing ,Virology ,A-site ,Epitope mapping ,chemistry ,Mutation ,biology.protein ,Glycoprotein ,Epitope Mapping ,030217 neurology & neurosurgery - Abstract
The SARS-CoV-2 spike (S) glycoprotein contains an immunodominant receptor-binding domain (RBD) targeted by most neutralizing antibodies (Abs) in COVID-19 patient plasma. Little is known about neutralizing Abs binding to epitopes outside the RBD and their contribution to protection. Here, we describe 41 human monoclonal Abs (mAbs) derived from memory B cells, which recognize the SARS-CoV-2 S N-terminal domain (NTD) and show that a subset of them neutralize SARS-CoV-2 ultrapotently. We define an antigenic map of the SARS-CoV-2 NTD and identify a supersite (designated site i) recognized by all known NTD-specific neutralizing mAbs. These mAbs inhibit cell-to-cell fusion, activate effector functions, and protect Syrian hamsters from SARS-CoV-2 challenge, albeit selecting escape mutants in some animals. Indeed, several SARS-CoV-2 variants, including the B.1.1.7, B.1.351 and P1 lineages, harbor frequent mutations within the NTD supersite suggesting ongoing selective pressure and the importance of NTD-specific neutralizing mAbs for protective immunity and vaccine design., McCallum et al. identify a supersite in the N-terminal domain of SARS-CoV-2 spike protein that is targeted by neutralizing antibodies and exhibits mutation in response to selective pressure.
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- 2021
13. Integrated approach for the analysis of some pesticides in vegetables and food matrices
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Fabbri, Debora, Calza, Paola, Anna, Dioni, Marco, Bergero, Barbara, Guarino, DAL BELLO, Federica, and Medana, Claudio
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- 2021
14. Mapping Neutralizing and Immunodominant Sites on the SARS-CoV-2 Spike Receptor-Binding Domain by Structure-Guided High-Resolution Serology
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Herbert W. Virgin, David K. Hong, Alessandra Franzetti Pellanda, John E. Bowen, Alessandro Ceschi, Andrea Minola, M. Alejandra Tortorici, Agostino Riva, Colin Havenar-Daughton, G. Snell, Paolo Ferrari, Nicole Sprugasci, Oliver J. Acton, Sneha V. Gupta, Luca Piccoli, Anna De Marco, Enos Bernasconi, Alexandra C. Walls, David Veesler, Nadine Czudnochowski, Antonio Lanzavecchia, Blanca Fernandez Rodriguez, Emiliano Albanese, Katja Fink, Barbara Guarino, Alessia Peter, Giovanni Piumatti, Stefano Jaconi, Maciej Tarkowski, Davide Corti, Christian Garzoni, Elisabetta Cameroni, Jessica Bassi, Laura E. Rosen, Chiara Silacci-Fregni, Valentino Lepori, Federica Sallusto, Dora Pinto, Federico Mele, Megan Smithey, Fabrizia Zatta, Feng Jin, Jay C. Nix, Sandra Jovic, Martina Beltramello, Matteo Samuele Pizzuto, Young-Jun Park, Maira Biggiogero, Luigia Elzi, Giorgia Lo Presti, Humabs BioMed SA, University of Washington [Seattle], Vir Biotechnology [San Francisco], Lawrence Berkeley National Laboratory [Berkeley] (LBNL), Università della Svizzera italiana = University of Italian Switzerland (USI), Clinica Luganese Moncucco [Lugano], Luigi Sacco University Hospital [Milan], Vir Biotechnology Inc [San Francisco], University hospital of Zurich [Zurich], Ospedale Civico and Ospedale Italiano [Lugano], Ospedale Regionale Bellinzona e Valli and Ospedale Regionale [Locarno], University of New South Wales [Sydney] (UNSW), and Institute for Research in Biomedicine
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Antibodies, Viral ,Medical and Health Sciences ,Immunoglobulin G ,Epitope ,Antigen-Antibody Reactions ,Epitopes ,0302 clinical medicine ,Monoclonal ,Viral ,Neutralizing ,Lung ,0303 health sciences ,biology ,Antibodies, Monoclonal ,Biological Sciences ,Spike Glycoprotein ,3. Good health ,Infectious Diseases ,Spike Glycoprotein, Coronavirus ,Pneumonia & Influenza ,Angiotensin-Converting Enzyme 2 ,Antibody ,Coronavirus Infections ,Infection ,Protein Binding ,Protein Structure ,coronaviruses ,Pneumonia, Viral ,Immunodominance ,Peptidyl-Dipeptidase A ,Molecular Dynamics Simulation ,Article ,General Biochemistry, Genetics and Molecular Biology ,Antibodies ,effector functions ,Affinity maturation ,Quaternary ,Vaccine Related ,03 medical and health sciences ,Betacoronavirus ,Antigen ,Protein Domains ,Clinical Research ,Biodefense ,Humans ,Avidity ,neutralizing antibodies ,[SDV.BBM]Life Sciences [q-bio]/Biochemistry, Molecular Biology ,Protein Structure, Quaternary ,Pandemics ,030304 developmental biology ,Binding Sites ,SARS-CoV-2 ,Prevention ,COVID-19 ,Pneumonia ,Antibodies, Neutralizing ,Virology ,immunity ,Immunoglobulin A ,Coronavirus ,Kinetics ,Epitope mapping ,Emerging Infectious Diseases ,Good Health and Well Being ,Immunoglobulin M ,biology.protein ,Immunization ,030217 neurology & neurosurgery ,Epitope Mapping ,Developmental Biology - Abstract
Analysis of the specificity and kinetics of neutralizing antibodies (nAbs) elicited by SARS-CoV-2 infection is crucial for understanding immune protection and identifying targets for vaccine design. In a cohort of 647 SARS-CoV-2-infected subjects, we found that both the magnitude of Ab responses to SARS-CoV-2 spike (S) and nucleoprotein and nAb titers correlate with clinical scores. The receptor-binding domain (RBD) is immunodominant and the target of 90% of the neutralizing activity present in SARS-CoV-2 immune sera. Whereas overall RBD-specific serum IgG titers waned with a half-life of 49 days, nAb titers and avidity increased over time for some individuals, consistent with affinity maturation. We structurally defined an RBD antigenic map and serologically quantified serum Abs specific for distinct RBD epitopes leading to the identification of two major receptor-binding motif antigenic sites. Our results explain the immunodominance of the receptor-binding motif and will guide the design of COVID-19 vaccines and therapeutics., Graphical Abstract, Highlights • SARS-CoV-2 RBD is immunodominant and accounts for 90% of serum neutralizing activity • RBD antibodies decline with a half-life of ∼50 days, but their avidity increases • Structural definition of a SARS-CoV-2 RBD antigenic map using monoclonal antibodies • ACE2-binding site dominates SARS-CoV-2 polyclonal neutralizing antibody responses, Serological analyses of ∼650 SARS-CoV-2-exposed individuals show that 90% of the serum or plasma neutralizing activity targets the virus receptor-binding domain, with structural insights revealing how distinct types of neutralizing antibodies targeting the ACE2-binding site dominate the immune response against SARS-CoV-2 spike.
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- 2020
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15. Ultrapotent human antibodies protect against SARS-CoV-2 challenge via multiple mechanisms
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Ha V. Dang, Andrea Minola, Michael A. Schmid, Cindy Ng, Rana Abdelnabi, Matthew McCallum, David Veesler, Heather Tucker, Alessia Peter, Michael S. Diamond, Katja Culap, Josh Dillen, Nicole Sprugasci, Jiayi Zhou, Martin Montiel-Ruiz, Hannah Kaiser, James Brett Case, M. Alejandra Tortorici, Roberto Spreafico, Marcel Meury, Siro Bianchi, Herbert W. Virgin, Jason A. Wojcechowskyj, Elisabetta Cameroni, John E. Bowen, Agostino Riva, Fabio Benigni, G. Snell, Massimo Galli, Barbara Guarino, Martina Beltramello, Colin Havenar-Daughton, Matteo Samuele Pizzuto, Stefano Jaconi, Davide Corti, Anna De Marco, Arianna Gabrieli, Rita E. Chen, Florian A. Lempp, Laura E. Rosen, Shi Yan Caroline Foo, Elvin J. Lauron, Katja Fink, Nadine Czudnochowski, Dora Pinto, Johan Neyts, and Fabrizia Zatta
- Subjects
0301 basic medicine ,Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) ,viruses ,Protein domain ,Mutant ,Amino Acid Motifs ,Pneumonia, Viral ,Immunology ,CHO Cells ,Biology ,Peptidyl-Dipeptidase A ,Antibodies, Viral ,Epitope ,03 medical and health sciences ,Betacoronavirus ,0302 clinical medicine ,Cricetulus ,Protein Domains ,Cricetinae ,Animals ,Humans ,Pandemics ,Research Articles ,Multidisciplinary ,Immunodominant Epitopes ,SARS-CoV-2 ,Chinese hamster ovary cell ,R-Articles ,HEK 293 cells ,fungi ,Cryoelectron Microscopy ,COVID-19 ,Biochem ,biology.organism_classification ,Virology ,Antibodies, Neutralizing ,Microscopy, Electron ,030104 developmental biology ,HEK293 Cells ,Spike Glycoprotein, Coronavirus ,biology.protein ,Angiotensin-Converting Enzyme 2 ,Antibody ,Coronavirus Infections ,030217 neurology & neurosurgery ,Research Article - Abstract
A strong cocktail against SARS-CoV-2 Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection is initiated by the trimeric spike protein that decorates the virus and binds the ACE2 receptor. Antibodies against the spike that neutralize viral infection have potential as therapeutics. Tortorici et al. describe two very potent antibodies, S2E12 and S2M11. Electron microscopy structures characterized the binding and showed that S2E12 traps the spike in a conformation that cannot bind ACE2. Both antibodies protected hamsters against SARS-CoV-2 challenge and may be useful in antibody cocktails to combat the virus and prevent the development of resistance. Science, this issue p. 950, A potent antibody cocktail blocks attachment of SARS-CoV-2 to the host receptor and activates a protective immune response., Efficient therapeutic options are needed to control the spread of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) that has caused more than 922,000 fatalities as of 13 September 2020. We report the isolation and characterization of two ultrapotent SARS-CoV-2 human neutralizing antibodies (S2E12 and S2M11) that protect hamsters against SARS-CoV-2 challenge. Cryo–electron microscopy structures show that S2E12 and S2M11 competitively block angiotensin-converting enzyme 2 (ACE2) attachment and that S2M11 also locks the spike in a closed conformation by recognition of a quaternary epitope spanning two adjacent receptor-binding domains. Antibody cocktails that include S2M11, S2E12, or the previously identified S309 antibody broadly neutralize a panel of circulating SARS-CoV-2 isolates and activate effector functions. Our results pave the way to implement antibody cocktails for prophylaxis or therapy, circumventing or limiting the emergence of viral escape mutants.
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- 2020
16. Structural and functional analysis of a potent sarbecovirus neutralizing antibody
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Dora Pinto, Young-Jun Park, Martina Beltramello, Alexandra C. Walls, M. Alejandra Tortorici, Siro Bianchi, Stefano Jaconi, Katja Culap, Fabrizia Zatta, Anna De Marco, Alessia Peter, Barbara Guarino, Roberto Spreafico, Elisabetta Cameroni, James Brett Case, Rita E. Chen, Colin Havenar-Daughton, Gyorgy Snell, Amalio Telenti, Herbert W. Virgin, Antonio Lanzavecchia, Michael S. Diamond, Katja Fink, David Veesler, and Davide Corti
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body regions ,0303 health sciences ,03 medical and health sciences ,0302 clinical medicine ,030220 oncology & carcinogenesis ,viruses ,fungi ,skin and connective tissue diseases ,Article ,3. Good health ,030304 developmental biology - Abstract
SARS-CoV-2 is a newly emerged coronavirus responsible for the current COVID-19 pandemic that has resulted in more than one million infections and 73,000 deaths1,2. Vaccine and therapeutic discovery efforts are paramount to curb the pandemic spread of this zoonotic virus. The SARS-CoV-2 spike (S) glycoprotein promotes entry into host cells and is the main target of neutralizing antibodies. Here we describe multiple monoclonal antibodies targeting SARS-CoV-2 S identified from memory B cells of a SARS survivor infected in 2003. One antibody, named S309, potently neutralizes SARS-CoV-2 and SARS-CoV pseudoviruses as well as authentic SARS-CoV-2 by engaging the S receptor-binding domain. Using cryo-electron microscopy and binding assays, we show that S309 recognizes a glycan-containing epitope that is conserved within the sarbecovirus subgenus, without competing with receptor attachment. Antibody cocktails including S309 along with other antibodies identified here further enhanced SARS-CoV-2 neutralization and may limit the emergence of neutralization-escape mutants. These results pave the way for using S309 and S309-containing antibody cocktails for prophylaxis in individuals at high risk of exposure or as a post-exposure therapy to limit or treat severe disease.
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- 2020
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17. Cross-neutralization of SARS-CoV-2 by a human monoclonal SARS-CoV antibody
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Anna De Marco, Michael S. Diamond, Herbert W. Virgin, M. Alejandra Tortorici, Fabrizia Zatta, Katja Culap, Siro Bianchi, Stefano Jaconi, Martina Beltramello, Colin Havenar-Daughton, Amalio Telenti, David Veesler, Antonio Lanzavecchia, Davide Corti, Barbara Guarino, Dora Pinto, Gyorgy Snell, James Brett Case, Alessia Peter, Rita E. Chen, Elisabetta Cameroni, Katja Fink, Young-Jun Park, Roberto Spreafico, Alexandra C. Walls, Humabs BioMed SA, Department of Biochemistry [Washington ], University of Washington [Seattle], Virologie Structurale - Structural Virology, Institut Pasteur [Paris] (IP)-Centre National de la Recherche Scientifique (CNRS), Vir Biotechnology Inc [San Francisco], Washington University School of Medicine in St. Louis, Washington University in Saint Louis (WUSTL), Scuola Universitaria Professionale della Svizzera italiana, and Centre National de la Recherche Scientifique (CNRS)-Institut Pasteur [Paris]
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Models, Molecular ,0301 basic medicine ,viruses ,[SDV]Life Sciences [q-bio] ,Antibodies, Viral ,Severe Acute Respiratory Syndrome ,medicine.disease_cause ,Epitope ,Neutralization ,0302 clinical medicine ,Chlorocebus aethiops ,skin and connective tissue diseases ,Coronavirus ,B-Lymphocytes ,Multidisciplinary ,biology ,Antibodies, Monoclonal ,virus diseases ,Entry into host ,3. Good health ,Killer Cells, Natural ,Severe acute respiratory syndrome-related coronavirus ,Spike Glycoprotein, Coronavirus ,Monoclonal ,Epitopes, B-Lymphocyte ,Angiotensin-Converting Enzyme 2 ,Antibody ,Coronavirus Infections ,medicine.drug_class ,Pneumonia, Viral ,Cross Reactions ,Peptidyl-Dipeptidase A ,Monoclonal antibody ,Betacoronavirus ,Immunoglobulin Fab Fragments ,03 medical and health sciences ,Neutralization Tests ,medicine ,Animals ,Humans ,Pandemics ,Vero Cells ,Immune Evasion ,SARS-CoV-2 ,Cryoelectron Microscopy ,fungi ,Antibody-Dependent Cell Cytotoxicity ,COVID-19 ,biology.organism_classification ,Antibodies, Neutralizing ,Virology ,body regions ,HEK293 Cells ,030104 developmental biology ,biology.protein ,Immunologic Memory ,030217 neurology & neurosurgery - Abstract
Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) is a newly emerged coronavirus that is responsible for the current pandemic of coronavirus disease 2019 (COVID-19), which has resulted in more than 3.7 million infections and 260,000 deaths as of 6 May 20201,2. Vaccine and therapeutic discovery efforts are paramount to curb the pandemic spread of this zoonotic virus. The SARS-CoV-2 spike (S) glycoprotein promotes entry into host cells and is the main target of neutralizing antibodies. Here we describe several monoclonal antibodies that target the S glycoprotein of SARS-CoV-2, which we identified from memory B cells of an individual who was infected with severe acute respiratory syndrome coronavirus (SARS-CoV) in 2003. One antibody (named S309) potently neutralizes SARS-CoV-2 and SARS-CoV pseudoviruses as well as authentic SARS-CoV-2, by engaging the receptor-binding domain of the S glycoprotein. Using cryo-electron microscopy and binding assays, we show that S309 recognizes an epitope containing a glycan that is conserved within the Sarbecovirus subgenus, without competing with receptor attachment. Antibody cocktails that include S309 in combination with other antibodies that we identified further enhanced SARS-CoV-2 neutralization, and may limit the emergence of neutralization-escape mutants. These results pave the way for using S309 and antibody cocktails containing S309 for prophylaxis in individuals at a high risk of exposure or as a post-exposure therapy to limit or treat severe disease.
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- 2020
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18. Tackling influenza with broadly neutralizing antibodies
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Nicole L. Kallewaard, Qing Zhu, Elisabetta Cameroni, Davide Corti, Antonio Lanzavecchia, and Barbara Guarino
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0301 basic medicine ,medicine.drug_class ,High variability ,Hemagglutinin Glycoproteins, Influenza Virus ,Monoclonal antibody ,medicine.disease_cause ,Antiviral Agents ,Article ,Autoimmunity ,Mice ,03 medical and health sciences ,0302 clinical medicine ,Immune system ,Orthomyxoviridae Infections ,Antibody Repertoire ,Virology ,Influenza, Human ,medicine ,Animals ,Humans ,biology ,Antibodies, Monoclonal ,Cancer ,Influenza a ,medicine.disease ,Antibodies, Neutralizing ,Influenza B virus ,030104 developmental biology ,Influenza A virus ,030220 oncology & carcinogenesis ,Immunology ,biology.protein ,Antibody - Abstract
Highlights • Broadly neutralizing antibodies against influenza A and B represents a safe and affordable alternative to convalescent plasma. • The large majority of broadly neutralizing antibodies target the stem region of HA. • Antiviral protection by anti-HA antibodies comprises both Fab- and Fc-dependent mechanisms. • Several broadly neutralizing antibodies are in development for the therapy of severe influenza infections., Monoclonal antibodies have revolutionized the treatment of several human diseases, including cancer, autoimmunity and inflammatory conditions and represent a new frontier for the treatment of infectious diseases. In the last decade, new methods have allowed the efficient interrogation of the human antibody repertoire from influenza immune individuals and the isolation of several monoclonal antibodies capable of dealing with the high variability of influenza viruses. Here, we will provide a comprehensive overview of the specificity, antiviral and immunological mechanisms of action and development into the clinic of broadly reactive monoclonal antibodies against influenza A and B viruses.
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- 2017
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19. 1231. VIR-2482: A potent and broadly neutralizing antibody for the prophylaxis of influenza A illness
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David K. Hong, Anna De Marco, Andrea Minola, Katja Culap, Alessia Peter, Christy M. Hebner, Matteo Samuele Pizzuto, Fabrizia Zatta, Aurelio Bonavia, Fabio Benigni, Nadia Passini, Davide Corti, Siro Bianchi, Leah Soriaga, and Barbara Guarino
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biology ,business.industry ,medicine.drug_class ,biochemical phenomena, metabolism, and nutrition ,medicine.disease_cause ,Monoclonal antibody ,Virology ,Neutralization ,Epitope ,Complement-dependent cytotoxicity ,AcademicSubjects/MED00290 ,Infectious Diseases ,Immune system ,Oncology ,Poster Abstracts ,Pandemic ,Influenza A virus ,medicine ,biology.protein ,bacteria ,Antibody ,business - Abstract
Background Influenza A viruses are responsible for seasonal epidemics and represent a constant pandemic threat. Influenza vaccines induce predominantly antibodies against the head region of hemagglutinin (HA) and are strain specific. Vaccine effectiveness is often suboptimal due to mismatch with drifting viruses and an inadequate immune response. Broadly neutralizing monoclonal antibodies (mAbs) targeting the conserved stem-region of HA may provide protection through multiple seasons and cover strains with pandemic potential. We report pre-clinical data on VIR-2482, a fully human anti-HA stem mAb with half-life extending Fc mutations. Methods Binding of VIR-2482 to a panel of influenza HAs and neutralization of H1N1 and H3N2 viruses were measured by ELISA and microneutralization. Epitope conservation was evaluated using 49,462 HA sequences retrieved from GiSAID. Engagement of human FcγRs by VIR-2482 was assessed by biolayer interferometry. Antibody-dependendent cell-mediated cytoxicity (ADCC) was measured via in vitro killing of A549 cells expressing H1-HA glycoprotein by human NK cells. Complement-dependent cytotoxicity (CDC) was evaluated by incubating VIR-2482 with H1N1 infected cells in the presence of guinea pig complement. Protection studies were performed in Balb/c mice given VIR-2482 24h before intranasal infection with a lethal dose of H1N1 PR8 and H3N2 HK/68. Results VIR-2482 binds to the HA proteins representing all 18 influenza A HA subtypes and neutralizes a broad panel of H1N1 and H3N2 viruses spanning almost 100 years of evolution. Bioinformatic analysis revealed >98.8% conservation for the majority of key contact residues examined from sequences retrieved for H1N1 and H3N2 between 2009-2019. The half-life extending mutations in the Fc portion do not affect the ability of the antibody to engage FcγRIIIa, FcγRIIa, and C1q as evidenced by their lack of impact on ADCC and CDC in vitro. Prophylactic administration of VIR-2482 protects Balb/c mice from infection with lethal challenge doses of H1N1 and H3N2 viruses. Conclusion The attributes of potency, broad recognition of a highly conserved epitope, retention of high-level effector functions in addition to half-life extension support the development of VIR-2482 as a universal prophylactic for influenza A illness. Disclosures Matteo Samuele Pizzuto, PhD, VIR Biotechnology (Employee) Fabrizia Zatta, n/a, Vir Biotechnology (Employee) Andrea Minola, MS, Vir Biotechnology (Employee) Alessia Peter, n/a, Vir Biotechnology (Employee) Katja Culap, n/a, Vir Biotechnology (Employee) Leah Soriaga, PhD, Vir Biotechnology (Employee) Anna De Marco, n/a, Vir Biotechnology (Employee) Barbara Guarino, PhD, Vir Biotechnology (Employee) Nadia Passini, n/a, Vir Biotechnology (Employee) David K. Hong, MD, Vir Biotechnology (Employee) Fabio Benigni, PhD, Vir Biotechnology (Employee) Christy Hebner, PhD, Vir Biotechnology (Employee) Aurelio Bonavia, PhD, Vir Biotechnology (Employee) Davide Corti, PhD, Vir Biotechnology (Employee)
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- 2020
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20. Structure and Function Analysis of an Antibody Recognizing All Influenza A Subtypes
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Barbara Guarino, Ursula Neu, Philip A. Walker, Patrick J. Collins, Frances J. Palmer-Hill, Josephine M. McAuliffe, Fabrizia Vanzetta, JoAnn Suzich, Anna De Marco, Stephen R. Martin, Roksana W. Ogrodowicz, Leslie Wachter-Rosati, Qing Zhu, Steven J. Gamblin, Gloria Agatic, Chiara Silacci, Andy Q. Yuan, Nicole L. Kallewaard, Debora Pinna, Mathilde Foglierini, Alexander Fruehwirth, Federica Sallusto, John J. Skehel, Matthias K. Vorlaender, Antonio Lanzavecchia, Ebony Benjamin, Davide Corti, Siro Bianchi, and Blanca Fernandez-Rodriguez
- Subjects
Influenzavirus A ,0301 basic medicine ,Oseltamivir ,Protein Conformation ,medicine.drug_class ,Hemagglutinin (influenza) ,Biology ,Antibodies, Monoclonal, Humanized ,Antibodies, Viral ,Crystallography, X-Ray ,Monoclonal antibody ,General Biochemistry, Genetics and Molecular Biology ,Virus ,Epitope ,Antigenic drift ,Neutralization ,Article ,Epitopes ,Mice ,03 medical and health sciences ,chemistry.chemical_compound ,Orthomyxoviridae Infections ,Antibody Specificity ,medicine ,Animals ,Humans ,Amino Acid Sequence ,Biochemistry, Genetics and Molecular Biology(all) ,Ferrets ,Antibodies, Monoclonal ,virus diseases ,Antibodies, Neutralizing ,Virology ,3. Good health ,030104 developmental biology ,chemistry ,Influenza Vaccines ,biology.protein ,Binding Sites, Antibody ,Antibody - Abstract
Summary Influenza virus remains a threat because of its ability to evade vaccine-induced immune responses due to antigenic drift. Here, we describe the isolation, evolution, and structure of a broad-spectrum human monoclonal antibody (mAb), MEDI8852, effectively reacting with all influenza A hemagglutinin (HA) subtypes. MEDI8852 uses the heavy-chain VH6-1 gene and has higher potency and breadth when compared to other anti-stem antibodies. MEDI8852 is effective in mice and ferrets with a therapeutic window superior to that of oseltamivir. Crystallographic analysis of Fab alone or in complex with H5 or H7 HA proteins reveals that MEDI8852 binds through a coordinated movement of CDRs to a highly conserved epitope encompassing a hydrophobic groove in the fusion domain and a large portion of the fusion peptide, distinguishing it from other structurally characterized cross-reactive antibodies. The unprecedented breadth and potency of neutralization by MEDI8852 support its development as immunotherapy for influenza virus-infected humans., Graphical Abstract, Highlights • Binding to all influenza A subtypes neutralizing seasonal and pandemic strains • Utilizes a rare VH (VH6-1) and carries a low level of somatic mutations • Highly conserved epitope encompassing fusion peptide and hydrophobic groove • Superior therapeutic window compared to oseltamivir in animals, Identification of a human monoclonal antibody that reacts effectively with all influenza A hemagglutinin subtypes paves the way for developing immunotherapy for people infected with the flu virus.
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- 2016
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