Potent neutralization of clinical isolates of SARS-CoV-2 D614 and G614 variants by a monomeric, sub-nanomolar affinity nanobody

Potent neutralization of clinical isolates of SARS-CoV-2 D614 and G614 variants by a monomeric, sub-nanomolar affinity nanobody

Abstract Despite unprecedented global efforts to rapidly develop SARS-CoV-2 treatments, in order to reduce the burden placed on health systems, the situation remains critical. Effective diagnosis, treatment, and prophylactic measures are urgently required to meet global demand: recombinant antibodie...

Full description

Bibliographic Details
Main Authors: Guillermo Valenzuela Nieto, Ronald Jara, Daniel Watterson, Naphak Modhiran, Alberto A. Amarilla, Johanna Himelreichs, Alexander A. Khromykh, Constanza Salinas-Rebolledo, Teresa Pinto, Yorka Cheuquemilla, Yago Margolles, Natalia López González del Rey, Zaray Miranda-Chacon, Alexei Cuevas, Anne Berking, Camila Deride, Sebastián González-Moraga, Héctor Mancilla, Daniel Maturana, Andreas Langer, Juan Pablo Toledo, Ananda Müller, Benjamín Uberti, Paola Krall, Pamela Ehrenfeld, Javier Blesa, Pedro Chana-Cuevas, German Rehren, David Schwefel, Luis Ángel Fernandez, Alejandro Rojas-Fernandez
Format: Article
Language:English
Published: Nature Publishing Group 2021-02-01
Series:Scientific Reports
Online Access:https://doi.org/10.1038/s41598-021-82833-w
id doaj-ee67da82c4154da782d61078ae559f70
record_format Article
collection DOAJ
language English
format Article
sources DOAJ
author Guillermo Valenzuela Nieto
Ronald Jara
Daniel Watterson
Naphak Modhiran
Alberto A. Amarilla
Johanna Himelreichs
Alexander A. Khromykh
Constanza Salinas-Rebolledo
Teresa Pinto
Yorka Cheuquemilla
Yago Margolles
Natalia López González del Rey
Zaray Miranda-Chacon
Alexei Cuevas
Anne Berking
Camila Deride
Sebastián González-Moraga
Héctor Mancilla
Daniel Maturana
Andreas Langer
Juan Pablo Toledo
Ananda Müller
Benjamín Uberti
Paola Krall
Pamela Ehrenfeld
Javier Blesa
Pedro Chana-Cuevas
German Rehren
David Schwefel
Luis Ángel Fernandez
Alejandro Rojas-Fernandez
spellingShingle Guillermo Valenzuela Nieto
Ronald Jara
Daniel Watterson
Naphak Modhiran
Alberto A. Amarilla
Johanna Himelreichs
Alexander A. Khromykh
Constanza Salinas-Rebolledo
Teresa Pinto
Yorka Cheuquemilla
Yago Margolles
Natalia López González del Rey
Zaray Miranda-Chacon
Alexei Cuevas
Anne Berking
Camila Deride
Sebastián González-Moraga
Héctor Mancilla
Daniel Maturana
Andreas Langer
Juan Pablo Toledo
Ananda Müller
Benjamín Uberti
Paola Krall
Pamela Ehrenfeld
Javier Blesa
Pedro Chana-Cuevas
German Rehren
David Schwefel
Luis Ángel Fernandez
Alejandro Rojas-Fernandez
Potent neutralization of clinical isolates of SARS-CoV-2 D614 and G614 variants by a monomeric, sub-nanomolar affinity nanobody
Scientific Reports
author_facet Guillermo Valenzuela Nieto
Ronald Jara
Daniel Watterson
Naphak Modhiran
Alberto A. Amarilla
Johanna Himelreichs
Alexander A. Khromykh
Constanza Salinas-Rebolledo
Teresa Pinto
Yorka Cheuquemilla
Yago Margolles
Natalia López González del Rey
Zaray Miranda-Chacon
Alexei Cuevas
Anne Berking
Camila Deride
Sebastián González-Moraga
Héctor Mancilla
Daniel Maturana
Andreas Langer
Juan Pablo Toledo
Ananda Müller
Benjamín Uberti
Paola Krall
Pamela Ehrenfeld
Javier Blesa
Pedro Chana-Cuevas
German Rehren
David Schwefel
Luis Ángel Fernandez
Alejandro Rojas-Fernandez
author_sort Guillermo Valenzuela Nieto
title Potent neutralization of clinical isolates of SARS-CoV-2 D614 and G614 variants by a monomeric, sub-nanomolar affinity nanobody
title_short Potent neutralization of clinical isolates of SARS-CoV-2 D614 and G614 variants by a monomeric, sub-nanomolar affinity nanobody
title_full Potent neutralization of clinical isolates of SARS-CoV-2 D614 and G614 variants by a monomeric, sub-nanomolar affinity nanobody
title_fullStr Potent neutralization of clinical isolates of SARS-CoV-2 D614 and G614 variants by a monomeric, sub-nanomolar affinity nanobody
title_full_unstemmed Potent neutralization of clinical isolates of SARS-CoV-2 D614 and G614 variants by a monomeric, sub-nanomolar affinity nanobody
title_sort potent neutralization of clinical isolates of sars-cov-2 d614 and g614 variants by a monomeric, sub-nanomolar affinity nanobody
publisher Nature Publishing Group
series Scientific Reports
issn 2045-2322
publishDate 2021-02-01
description Abstract Despite unprecedented global efforts to rapidly develop SARS-CoV-2 treatments, in order to reduce the burden placed on health systems, the situation remains critical. Effective diagnosis, treatment, and prophylactic measures are urgently required to meet global demand: recombinant antibodies fulfill these requirements and have marked clinical potential. Here, we describe the fast-tracked development of an alpaca Nanobody specific for the receptor-binding-domain (RBD) of the SARS-CoV-2 Spike protein with potential therapeutic applicability. We present a rapid method for nanobody isolation that includes an optimized immunization regimen coupled with VHH library E. coli surface display, which allows single-step selection of Nanobodies using a simple density gradient centrifugation of the bacterial library. The selected single and monomeric Nanobody, W25, binds to the SARS-CoV-2 S RBD with sub-nanomolar affinity and efficiently competes with ACE-2 receptor binding. Furthermore, W25 potently neutralizes SARS-CoV-2 wild type and the D614G variant with IC50 values in the nanomolar range, demonstrating its potential as antiviral agent.
url https://doi.org/10.1038/s41598-021-82833-w
work_keys_str_mv AT guillermovalenzuelanieto potentneutralizationofclinicalisolatesofsarscov2d614andg614variantsbyamonomericsubnanomolaraffinitynanobody
AT ronaldjara potentneutralizationofclinicalisolatesofsarscov2d614andg614variantsbyamonomericsubnanomolaraffinitynanobody
AT danielwatterson potentneutralizationofclinicalisolatesofsarscov2d614andg614variantsbyamonomericsubnanomolaraffinitynanobody
AT naphakmodhiran potentneutralizationofclinicalisolatesofsarscov2d614andg614variantsbyamonomericsubnanomolaraffinitynanobody
AT albertoaamarilla potentneutralizationofclinicalisolatesofsarscov2d614andg614variantsbyamonomericsubnanomolaraffinitynanobody
AT johannahimelreichs potentneutralizationofclinicalisolatesofsarscov2d614andg614variantsbyamonomericsubnanomolaraffinitynanobody
AT alexanderakhromykh potentneutralizationofclinicalisolatesofsarscov2d614andg614variantsbyamonomericsubnanomolaraffinitynanobody
AT constanzasalinasrebolledo potentneutralizationofclinicalisolatesofsarscov2d614andg614variantsbyamonomericsubnanomolaraffinitynanobody
AT teresapinto potentneutralizationofclinicalisolatesofsarscov2d614andg614variantsbyamonomericsubnanomolaraffinitynanobody
AT yorkacheuquemilla potentneutralizationofclinicalisolatesofsarscov2d614andg614variantsbyamonomericsubnanomolaraffinitynanobody
AT yagomargolles potentneutralizationofclinicalisolatesofsarscov2d614andg614variantsbyamonomericsubnanomolaraffinitynanobody
AT natalialopezgonzalezdelrey potentneutralizationofclinicalisolatesofsarscov2d614andg614variantsbyamonomericsubnanomolaraffinitynanobody
AT zaraymirandachacon potentneutralizationofclinicalisolatesofsarscov2d614andg614variantsbyamonomericsubnanomolaraffinitynanobody
AT alexeicuevas potentneutralizationofclinicalisolatesofsarscov2d614andg614variantsbyamonomericsubnanomolaraffinitynanobody
AT anneberking potentneutralizationofclinicalisolatesofsarscov2d614andg614variantsbyamonomericsubnanomolaraffinitynanobody
AT camiladeride potentneutralizationofclinicalisolatesofsarscov2d614andg614variantsbyamonomericsubnanomolaraffinitynanobody
AT sebastiangonzalezmoraga potentneutralizationofclinicalisolatesofsarscov2d614andg614variantsbyamonomericsubnanomolaraffinitynanobody
AT hectormancilla potentneutralizationofclinicalisolatesofsarscov2d614andg614variantsbyamonomericsubnanomolaraffinitynanobody
AT danielmaturana potentneutralizationofclinicalisolatesofsarscov2d614andg614variantsbyamonomericsubnanomolaraffinitynanobody
AT andreaslanger potentneutralizationofclinicalisolatesofsarscov2d614andg614variantsbyamonomericsubnanomolaraffinitynanobody
AT juanpablotoledo potentneutralizationofclinicalisolatesofsarscov2d614andg614variantsbyamonomericsubnanomolaraffinitynanobody
AT anandamuller potentneutralizationofclinicalisolatesofsarscov2d614andg614variantsbyamonomericsubnanomolaraffinitynanobody
AT benjaminuberti potentneutralizationofclinicalisolatesofsarscov2d614andg614variantsbyamonomericsubnanomolaraffinitynanobody
AT paolakrall potentneutralizationofclinicalisolatesofsarscov2d614andg614variantsbyamonomericsubnanomolaraffinitynanobody
AT pamelaehrenfeld potentneutralizationofclinicalisolatesofsarscov2d614andg614variantsbyamonomericsubnanomolaraffinitynanobody
AT javierblesa potentneutralizationofclinicalisolatesofsarscov2d614andg614variantsbyamonomericsubnanomolaraffinitynanobody
AT pedrochanacuevas potentneutralizationofclinicalisolatesofsarscov2d614andg614variantsbyamonomericsubnanomolaraffinitynanobody
AT germanrehren potentneutralizationofclinicalisolatesofsarscov2d614andg614variantsbyamonomericsubnanomolaraffinitynanobody
AT davidschwefel potentneutralizationofclinicalisolatesofsarscov2d614andg614variantsbyamonomericsubnanomolaraffinitynanobody
AT luisangelfernandez potentneutralizationofclinicalisolatesofsarscov2d614andg614variantsbyamonomericsubnanomolaraffinitynanobody
AT alejandrorojasfernandez potentneutralizationofclinicalisolatesofsarscov2d614andg614variantsbyamonomericsubnanomolaraffinitynanobody
_version_ 1724270344273920000
spelling doaj-ee67da82c4154da782d61078ae559f702021-02-14T12:32:27ZengNature Publishing GroupScientific Reports2045-23222021-02-0111111410.1038/s41598-021-82833-wPotent neutralization of clinical isolates of SARS-CoV-2 D614 and G614 variants by a monomeric, sub-nanomolar affinity nanobodyGuillermo Valenzuela Nieto0Ronald Jara1Daniel Watterson2Naphak Modhiran3Alberto A. Amarilla4Johanna Himelreichs5Alexander A. Khromykh6Constanza Salinas-Rebolledo7Teresa Pinto8Yorka Cheuquemilla9Yago Margolles10Natalia López González del Rey11Zaray Miranda-Chacon12Alexei Cuevas13Anne Berking14Camila Deride15Sebastián González-Moraga16Héctor Mancilla17Daniel Maturana18Andreas Langer19Juan Pablo Toledo20Ananda Müller21Benjamín Uberti22Paola Krall23Pamela Ehrenfeld24Javier Blesa25Pedro Chana-Cuevas26German Rehren27David Schwefel28Luis Ángel Fernandez29Alejandro Rojas-Fernandez30Institute of Medicine, Faculty of Medicine, Universidad Austral de ChileInstitute of Medicine, Faculty of Medicine, Universidad Austral de ChileSchool of Chemistry and Molecular Bioscience, The University of QueenslandSchool of Chemistry and Molecular Bioscience, The University of QueenslandSchool of Chemistry and Molecular Bioscience, The University of QueenslandInstitute of Medicine, Faculty of Medicine, Universidad Austral de ChileSchool of Chemistry and Molecular Bioscience, The University of QueenslandInstitute of Medicine, Faculty of Medicine, Universidad Austral de ChileInstitute of Medicine, Faculty of Medicine, Universidad Austral de ChileInstitute of Medicine, Faculty of Medicine, Universidad Austral de ChileDepartment of Microbial Biotechnology, National Biotechnology Center, Superior Council of Scientific ResearchHM CINAC, Hospital Universitario HM Puerta del SurInstitute of Medicine, Faculty of Medicine, Universidad Austral de ChileInstitute of Medicine, Faculty of Medicine, Universidad Austral de ChileBerking BiotechnologyInstitute of Medicine, Faculty of Medicine, Universidad Austral de ChileInstitute of Medicine, Faculty of Medicine, Universidad Austral de ChileInstitute of Medicine, Faculty of Medicine, Universidad Austral de ChileNanoTemper Technologies GmbHNanoTemper Technologies GmbHInstitute of Medicine, Faculty of Medicine, Universidad Austral de ChileRoss University School of Veterinary MedicineInstitute of Veterinary Clinical Sciences, Faculty of Veterinary Sciences, Universidad Austral de ChileInstitute of Medicine, Faculty of Medicine, Universidad Austral de ChileInstitute of Anatomy, Histology, and Pathology, Faculty of Medicine, Universidad Austral de ChileHM CINAC, Hospital Universitario HM Puerta del SurCETRAM & Faculty of Medical Science, Universidad de Santiago de ChileTechnology Transfer and Licensing Office, Universidad Austral de ChileCharité-Universitätsmedizin Berlin, Corporate Member of Freie Universität Berlin, Humboldt-Universität zu Berlin, Berlin Institute of HealthDepartment of Microbial Biotechnology, National Biotechnology Center, Superior Council of Scientific ResearchInstitute of Medicine, Faculty of Medicine, Universidad Austral de ChileAbstract Despite unprecedented global efforts to rapidly develop SARS-CoV-2 treatments, in order to reduce the burden placed on health systems, the situation remains critical. Effective diagnosis, treatment, and prophylactic measures are urgently required to meet global demand: recombinant antibodies fulfill these requirements and have marked clinical potential. Here, we describe the fast-tracked development of an alpaca Nanobody specific for the receptor-binding-domain (RBD) of the SARS-CoV-2 Spike protein with potential therapeutic applicability. We present a rapid method for nanobody isolation that includes an optimized immunization regimen coupled with VHH library E. coli surface display, which allows single-step selection of Nanobodies using a simple density gradient centrifugation of the bacterial library. The selected single and monomeric Nanobody, W25, binds to the SARS-CoV-2 S RBD with sub-nanomolar affinity and efficiently competes with ACE-2 receptor binding. Furthermore, W25 potently neutralizes SARS-CoV-2 wild type and the D614G variant with IC50 values in the nanomolar range, demonstrating its potential as antiviral agent.https://doi.org/10.1038/s41598-021-82833-w

Similar Items