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An ultra-potent synthetic nanobody neutralizes SARS-CoV-2 by locking Spike into an inactive conformation

Without an effective prophylactic solution, infections from SARS-CoV-2 continue to rise worldwide with devastating health and economic costs. SARS-CoV-2 gains entry into host cells via an interaction between its Spike protein and the host cell receptor angiotensin converting enzyme 2 (ACE2). Disrupt...

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Autores principales: Schoof, Michael, Faust, Bryan, Saunders, Reuben A., Sangwan, Smriti, Rezelj, Veronica, Hoppe, Nick, Boone, Morgane, Billesbølle, Christian B., Puchades, Cristina, Azumaya, Caleigh M., Kratochvil, Huong T., Zimanyi, Marcell, Deshpande, Ishan, Liang, Jiahao, Dickinson, Sasha, Nguyen, Henry C., Chio, Cynthia M., Merz, Gregory E., Thompson, Michael C., Diwanji, Devan, Schaefer, Kaitlin, Anand, Aditya A., Dobzinski, Niv, Zha, Beth Shoshana, Simoneau, Camille R., Leon, Kristoffer, White, Kris M., Chio, Un Seng, Gupta, Meghna, Jin, Mingliang, Li, Fei, Liu, Yanxin, Zhang, Kaihua, Bulkley, David, Sun, Ming, Smith, Amber M., Rizo, Alexandrea N., Moss, Frank, Brilot, Axel F., Pourmal, Sergei, Trenker, Raphael, Pospiech, Thomas, Gupta, Sayan, Barsi-Rhyne, Benjamin, Belyy, Vladislav, Barile-Hill, Andrew W., Nock, Silke, Liu, Yuwei, Krogan, Nevan J., Ralston, Corie Y., Swaney, Danielle L., García-Sastre, Adolfo, Ott, Melanie, Vignuzzi, Marco, Walter, Peter, Manglik, Aashish
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Cold Spring Harbor Laboratory 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7430568/
https://www.ncbi.nlm.nih.gov/pubmed/32817938
http://dx.doi.org/10.1101/2020.08.08.238469
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author Schoof, Michael
Faust, Bryan
Saunders, Reuben A.
Sangwan, Smriti
Rezelj, Veronica
Hoppe, Nick
Boone, Morgane
Billesbølle, Christian B.
Puchades, Cristina
Azumaya, Caleigh M.
Kratochvil, Huong T.
Zimanyi, Marcell
Deshpande, Ishan
Liang, Jiahao
Dickinson, Sasha
Nguyen, Henry C.
Chio, Cynthia M.
Merz, Gregory E.
Thompson, Michael C.
Diwanji, Devan
Schaefer, Kaitlin
Anand, Aditya A.
Dobzinski, Niv
Zha, Beth Shoshana
Simoneau, Camille R.
Leon, Kristoffer
White, Kris M.
Chio, Un Seng
Gupta, Meghna
Jin, Mingliang
Li, Fei
Liu, Yanxin
Zhang, Kaihua
Bulkley, David
Sun, Ming
Smith, Amber M.
Rizo, Alexandrea N.
Moss, Frank
Brilot, Axel F.
Pourmal, Sergei
Trenker, Raphael
Pospiech, Thomas
Gupta, Sayan
Barsi-Rhyne, Benjamin
Belyy, Vladislav
Barile-Hill, Andrew W.
Nock, Silke
Liu, Yuwei
Krogan, Nevan J.
Ralston, Corie Y.
Swaney, Danielle L.
García-Sastre, Adolfo
Ott, Melanie
Vignuzzi, Marco
Walter, Peter
Manglik, Aashish
author_facet Schoof, Michael
Faust, Bryan
Saunders, Reuben A.
Sangwan, Smriti
Rezelj, Veronica
Hoppe, Nick
Boone, Morgane
Billesbølle, Christian B.
Puchades, Cristina
Azumaya, Caleigh M.
Kratochvil, Huong T.
Zimanyi, Marcell
Deshpande, Ishan
Liang, Jiahao
Dickinson, Sasha
Nguyen, Henry C.
Chio, Cynthia M.
Merz, Gregory E.
Thompson, Michael C.
Diwanji, Devan
Schaefer, Kaitlin
Anand, Aditya A.
Dobzinski, Niv
Zha, Beth Shoshana
Simoneau, Camille R.
Leon, Kristoffer
White, Kris M.
Chio, Un Seng
Gupta, Meghna
Jin, Mingliang
Li, Fei
Liu, Yanxin
Zhang, Kaihua
Bulkley, David
Sun, Ming
Smith, Amber M.
Rizo, Alexandrea N.
Moss, Frank
Brilot, Axel F.
Pourmal, Sergei
Trenker, Raphael
Pospiech, Thomas
Gupta, Sayan
Barsi-Rhyne, Benjamin
Belyy, Vladislav
Barile-Hill, Andrew W.
Nock, Silke
Liu, Yuwei
Krogan, Nevan J.
Ralston, Corie Y.
Swaney, Danielle L.
García-Sastre, Adolfo
Ott, Melanie
Vignuzzi, Marco
Walter, Peter
Manglik, Aashish
author_sort Schoof, Michael
collection PubMed
description Without an effective prophylactic solution, infections from SARS-CoV-2 continue to rise worldwide with devastating health and economic costs. SARS-CoV-2 gains entry into host cells via an interaction between its Spike protein and the host cell receptor angiotensin converting enzyme 2 (ACE2). Disruption of this interaction confers potent neutralization of viral entry, providing an avenue for vaccine design and for therapeutic antibodies. Here, we develop single-domain antibodies (nanobodies) that potently disrupt the interaction between the SARS-CoV-2 Spike and ACE2. By screening a yeast surface-displayed library of synthetic nanobody sequences, we identified a panel of nanobodies that bind to multiple epitopes on Spike and block ACE2 interaction via two distinct mechanisms. Cryogenic electron microscopy (cryo-EM) revealed that one exceptionally stable nanobody, Nb6, binds Spike in a fully inactive conformation with its receptor binding domains (RBDs) locked into their inaccessible down-state, incapable of binding ACE2. Affinity maturation and structure-guided design of multivalency yielded a trivalent nanobody, mNb6-tri, with femtomolar affinity for SARS-CoV-2 Spike and picomolar neutralization of SARS-CoV-2 infection. mNb6-tri retains stability and function after aerosolization, lyophilization, and heat treatment. These properties may enable aerosol-mediated delivery of this potent neutralizer directly to the airway epithelia, promising to yield a widely deployable, patient-friendly prophylactic and/or early infection therapeutic agent to stem the worst pandemic in a century.
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spelling pubmed-74305682020-08-18 An ultra-potent synthetic nanobody neutralizes SARS-CoV-2 by locking Spike into an inactive conformation Schoof, Michael Faust, Bryan Saunders, Reuben A. Sangwan, Smriti Rezelj, Veronica Hoppe, Nick Boone, Morgane Billesbølle, Christian B. Puchades, Cristina Azumaya, Caleigh M. Kratochvil, Huong T. Zimanyi, Marcell Deshpande, Ishan Liang, Jiahao Dickinson, Sasha Nguyen, Henry C. Chio, Cynthia M. Merz, Gregory E. Thompson, Michael C. Diwanji, Devan Schaefer, Kaitlin Anand, Aditya A. Dobzinski, Niv Zha, Beth Shoshana Simoneau, Camille R. Leon, Kristoffer White, Kris M. Chio, Un Seng Gupta, Meghna Jin, Mingliang Li, Fei Liu, Yanxin Zhang, Kaihua Bulkley, David Sun, Ming Smith, Amber M. Rizo, Alexandrea N. Moss, Frank Brilot, Axel F. Pourmal, Sergei Trenker, Raphael Pospiech, Thomas Gupta, Sayan Barsi-Rhyne, Benjamin Belyy, Vladislav Barile-Hill, Andrew W. Nock, Silke Liu, Yuwei Krogan, Nevan J. Ralston, Corie Y. Swaney, Danielle L. García-Sastre, Adolfo Ott, Melanie Vignuzzi, Marco Walter, Peter Manglik, Aashish bioRxiv Article Without an effective prophylactic solution, infections from SARS-CoV-2 continue to rise worldwide with devastating health and economic costs. SARS-CoV-2 gains entry into host cells via an interaction between its Spike protein and the host cell receptor angiotensin converting enzyme 2 (ACE2). Disruption of this interaction confers potent neutralization of viral entry, providing an avenue for vaccine design and for therapeutic antibodies. Here, we develop single-domain antibodies (nanobodies) that potently disrupt the interaction between the SARS-CoV-2 Spike and ACE2. By screening a yeast surface-displayed library of synthetic nanobody sequences, we identified a panel of nanobodies that bind to multiple epitopes on Spike and block ACE2 interaction via two distinct mechanisms. Cryogenic electron microscopy (cryo-EM) revealed that one exceptionally stable nanobody, Nb6, binds Spike in a fully inactive conformation with its receptor binding domains (RBDs) locked into their inaccessible down-state, incapable of binding ACE2. Affinity maturation and structure-guided design of multivalency yielded a trivalent nanobody, mNb6-tri, with femtomolar affinity for SARS-CoV-2 Spike and picomolar neutralization of SARS-CoV-2 infection. mNb6-tri retains stability and function after aerosolization, lyophilization, and heat treatment. These properties may enable aerosol-mediated delivery of this potent neutralizer directly to the airway epithelia, promising to yield a widely deployable, patient-friendly prophylactic and/or early infection therapeutic agent to stem the worst pandemic in a century. Cold Spring Harbor Laboratory 2020-08-17 /pmc/articles/PMC7430568/ /pubmed/32817938 http://dx.doi.org/10.1101/2020.08.08.238469 Text en https://creativecommons.org/licenses/by-nc-nd/4.0/This work is licensed under a Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International License (https://creativecommons.org/licenses/by-nc-nd/4.0/) , which allows reusers to copy and distribute the material in any medium or format in unadapted form only, for noncommercial purposes only, and only so long as attribution is given to the creator.
spellingShingle Article
Schoof, Michael
Faust, Bryan
Saunders, Reuben A.
Sangwan, Smriti
Rezelj, Veronica
Hoppe, Nick
Boone, Morgane
Billesbølle, Christian B.
Puchades, Cristina
Azumaya, Caleigh M.
Kratochvil, Huong T.
Zimanyi, Marcell
Deshpande, Ishan
Liang, Jiahao
Dickinson, Sasha
Nguyen, Henry C.
Chio, Cynthia M.
Merz, Gregory E.
Thompson, Michael C.
Diwanji, Devan
Schaefer, Kaitlin
Anand, Aditya A.
Dobzinski, Niv
Zha, Beth Shoshana
Simoneau, Camille R.
Leon, Kristoffer
White, Kris M.
Chio, Un Seng
Gupta, Meghna
Jin, Mingliang
Li, Fei
Liu, Yanxin
Zhang, Kaihua
Bulkley, David
Sun, Ming
Smith, Amber M.
Rizo, Alexandrea N.
Moss, Frank
Brilot, Axel F.
Pourmal, Sergei
Trenker, Raphael
Pospiech, Thomas
Gupta, Sayan
Barsi-Rhyne, Benjamin
Belyy, Vladislav
Barile-Hill, Andrew W.
Nock, Silke
Liu, Yuwei
Krogan, Nevan J.
Ralston, Corie Y.
Swaney, Danielle L.
García-Sastre, Adolfo
Ott, Melanie
Vignuzzi, Marco
Walter, Peter
Manglik, Aashish
An ultra-potent synthetic nanobody neutralizes SARS-CoV-2 by locking Spike into an inactive conformation
title An ultra-potent synthetic nanobody neutralizes SARS-CoV-2 by locking Spike into an inactive conformation
title_full An ultra-potent synthetic nanobody neutralizes SARS-CoV-2 by locking Spike into an inactive conformation
title_fullStr An ultra-potent synthetic nanobody neutralizes SARS-CoV-2 by locking Spike into an inactive conformation
title_full_unstemmed An ultra-potent synthetic nanobody neutralizes SARS-CoV-2 by locking Spike into an inactive conformation
title_short An ultra-potent synthetic nanobody neutralizes SARS-CoV-2 by locking Spike into an inactive conformation
title_sort ultra-potent synthetic nanobody neutralizes sars-cov-2 by locking spike into an inactive conformation
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7430568/
https://www.ncbi.nlm.nih.gov/pubmed/32817938
http://dx.doi.org/10.1101/2020.08.08.238469
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