1348. Identification of GB-0669, a Novel S-2 Targeted Spike Monoclonal Antibody in Development for SARS-CoV-2 Prophylaxis

BACKGROUND: The clinical benefit of anti-spike mAbs for prophylaxis and treatment of SARS-CoV-2 is now well established (Baum 2020, Loo 2022, Westendorf 2022, Jones 2021, Kreuzberger 2021, Cathcart 2021, Hirsch 2022, Shi 2020); However, the evolution of SARS CoV-2 due to immune pressure has compromi...

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Autores principales: Borriello, Francesco, Marden, Grace, Li, Hongru, Carlin, Eric, Sharma, Geetika, Menzenski, Monica, Jecrois, Anne, Palovcak, Eugene, Lord, Dana, Tao, Jenhan, Grigoryan, Gevorg, Root, Adam, Hopson, Kristen, Hazuda, Daria, Van Epps, Heather A, Ramos, Alex, Joh, Nathan H, Russell, Pamela, Garlick, Joseph D
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2023
Materias:
Abstract
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10677384/
http://dx.doi.org/10.1093/ofid/ofad500.1185
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author Borriello, Francesco
Marden, Grace
Li, Hongru
Carlin, Eric
Sharma, Geetika
Menzenski, Monica
Jecrois, Anne
Palovcak, Eugene
Lord, Dana
Tao, Jenhan
Grigoryan, Gevorg
Root, Adam
Hopson, Kristen
Hazuda, Daria
Van Epps, Heather A
Ramos, Alex
Joh, Nathan H
Russell, Pamela
Garlick, Joseph D
author_facet Borriello, Francesco
Marden, Grace
Li, Hongru
Carlin, Eric
Sharma, Geetika
Menzenski, Monica
Jecrois, Anne
Palovcak, Eugene
Lord, Dana
Tao, Jenhan
Grigoryan, Gevorg
Root, Adam
Hopson, Kristen
Hazuda, Daria
Van Epps, Heather A
Ramos, Alex
Joh, Nathan H
Russell, Pamela
Garlick, Joseph D
author_sort Borriello, Francesco
collection PubMed
description BACKGROUND: The clinical benefit of anti-spike mAbs for prophylaxis and treatment of SARS-CoV-2 is now well established (Baum 2020, Loo 2022, Westendorf 2022, Jones 2021, Kreuzberger 2021, Cathcart 2021, Hirsch 2022, Shi 2020); However, the evolution of SARS CoV-2 due to immune pressure has compromised the utility of all previously approved mAbs which target the variable, immune dominant receptor binding domain of the Spike protein. Despite the success of vaccination protecting the general population, the immunocompromised and elderly remain at high risk of serious disease and mortality from SARS CoV-2 infection. Therefore, there is a need to develop mAbs that remain active across current and emergent SARS CoV-2 variants for such populations. METHODS: The Generate Platform uses machine learning (ML) models to generate therapeutics with desirable properties. We used this platform to explore the amino acid sequence landscape compatible with the binding conformation and breadth of neutralization for mAbs targeting the conserved S-2 stem helix of Spike. While S-2 directed antibodies can broadly neutralize diverse coronaviruses, they are generally limited by potency. We employed an iterative computation- experimentation loop to design antibodies that bind to the S-2 stem helix, optimizing for potency, breadth and developability. RESULTS: The Generate Platform was employed to identify S-2 targeted Spike antibodies with high potency and breadth of neutralization resulting in GB-0669. GB-0669 exhibits sub-nM neutralization against all SARS-CoV-2 variants and Omicron sublineages including the highly immune evasive strain XBB. GB-0669 also displays sub-nM neutralization against sarbecoviruses associated with previous epidemics (SARS-CoV-1) and those of pandemic potential (WIV1, bat SARS-like coronavirus). The GB 0669 epitope was mapped by co-crystallization and is consistent with the observed breadth; all key interactions are >99% conserved with no evidence of immune escape. CONCLUSION: GB-0669, a novel mAB targeting the conserved S-2 region of Spike, is hypothesized to be effective for prophylaxis of COVID-19 across all Omicron sublineages and future variants as well as CoVs with pandemic potential. DISCLOSURES: Francesco Borriello, MD PhD, Generate Biomedicines: Employee Gevorg Grigoryan, PhD, Generate Biomedicines: Chief Technology Officer|Generate Biomedicines: Ownership Interest|Generate Biomedicines: Stocks/Bonds Daria Hazuda, PhD, Generate Biomedicines: Employee|Generate Biomedicines: Stocks/Bonds|Merck and Co: Employee|Merck and Co: Stocks/Bonds Nathan H. Joh, PhD, Generate Biomedicines: Employee at Generate Biomedicines
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spelling pubmed-106773842023-11-27 1348. Identification of GB-0669, a Novel S-2 Targeted Spike Monoclonal Antibody in Development for SARS-CoV-2 Prophylaxis Borriello, Francesco Marden, Grace Li, Hongru Carlin, Eric Sharma, Geetika Menzenski, Monica Jecrois, Anne Palovcak, Eugene Lord, Dana Tao, Jenhan Grigoryan, Gevorg Root, Adam Hopson, Kristen Hazuda, Daria Van Epps, Heather A Ramos, Alex Joh, Nathan H Russell, Pamela Garlick, Joseph D Open Forum Infect Dis Abstract BACKGROUND: The clinical benefit of anti-spike mAbs for prophylaxis and treatment of SARS-CoV-2 is now well established (Baum 2020, Loo 2022, Westendorf 2022, Jones 2021, Kreuzberger 2021, Cathcart 2021, Hirsch 2022, Shi 2020); However, the evolution of SARS CoV-2 due to immune pressure has compromised the utility of all previously approved mAbs which target the variable, immune dominant receptor binding domain of the Spike protein. Despite the success of vaccination protecting the general population, the immunocompromised and elderly remain at high risk of serious disease and mortality from SARS CoV-2 infection. Therefore, there is a need to develop mAbs that remain active across current and emergent SARS CoV-2 variants for such populations. METHODS: The Generate Platform uses machine learning (ML) models to generate therapeutics with desirable properties. We used this platform to explore the amino acid sequence landscape compatible with the binding conformation and breadth of neutralization for mAbs targeting the conserved S-2 stem helix of Spike. While S-2 directed antibodies can broadly neutralize diverse coronaviruses, they are generally limited by potency. We employed an iterative computation- experimentation loop to design antibodies that bind to the S-2 stem helix, optimizing for potency, breadth and developability. RESULTS: The Generate Platform was employed to identify S-2 targeted Spike antibodies with high potency and breadth of neutralization resulting in GB-0669. GB-0669 exhibits sub-nM neutralization against all SARS-CoV-2 variants and Omicron sublineages including the highly immune evasive strain XBB. GB-0669 also displays sub-nM neutralization against sarbecoviruses associated with previous epidemics (SARS-CoV-1) and those of pandemic potential (WIV1, bat SARS-like coronavirus). The GB 0669 epitope was mapped by co-crystallization and is consistent with the observed breadth; all key interactions are >99% conserved with no evidence of immune escape. CONCLUSION: GB-0669, a novel mAB targeting the conserved S-2 region of Spike, is hypothesized to be effective for prophylaxis of COVID-19 across all Omicron sublineages and future variants as well as CoVs with pandemic potential. DISCLOSURES: Francesco Borriello, MD PhD, Generate Biomedicines: Employee Gevorg Grigoryan, PhD, Generate Biomedicines: Chief Technology Officer|Generate Biomedicines: Ownership Interest|Generate Biomedicines: Stocks/Bonds Daria Hazuda, PhD, Generate Biomedicines: Employee|Generate Biomedicines: Stocks/Bonds|Merck and Co: Employee|Merck and Co: Stocks/Bonds Nathan H. Joh, PhD, Generate Biomedicines: Employee at Generate Biomedicines Oxford University Press 2023-11-27 /pmc/articles/PMC10677384/ http://dx.doi.org/10.1093/ofid/ofad500.1185 Text en © The Author(s) 2023. Published by Oxford University Press on behalf of Infectious Diseases Society of America. https://creativecommons.org/licenses/by/4.0/This is an Open Access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/), which permits unrestricted reuse, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Abstract
Borriello, Francesco
Marden, Grace
Li, Hongru
Carlin, Eric
Sharma, Geetika
Menzenski, Monica
Jecrois, Anne
Palovcak, Eugene
Lord, Dana
Tao, Jenhan
Grigoryan, Gevorg
Root, Adam
Hopson, Kristen
Hazuda, Daria
Van Epps, Heather A
Ramos, Alex
Joh, Nathan H
Russell, Pamela
Garlick, Joseph D
1348. Identification of GB-0669, a Novel S-2 Targeted Spike Monoclonal Antibody in Development for SARS-CoV-2 Prophylaxis
title 1348. Identification of GB-0669, a Novel S-2 Targeted Spike Monoclonal Antibody in Development for SARS-CoV-2 Prophylaxis
title_full 1348. Identification of GB-0669, a Novel S-2 Targeted Spike Monoclonal Antibody in Development for SARS-CoV-2 Prophylaxis
title_fullStr 1348. Identification of GB-0669, a Novel S-2 Targeted Spike Monoclonal Antibody in Development for SARS-CoV-2 Prophylaxis
title_full_unstemmed 1348. Identification of GB-0669, a Novel S-2 Targeted Spike Monoclonal Antibody in Development for SARS-CoV-2 Prophylaxis
title_short 1348. Identification of GB-0669, a Novel S-2 Targeted Spike Monoclonal Antibody in Development for SARS-CoV-2 Prophylaxis
title_sort 1348. identification of gb-0669, a novel s-2 targeted spike monoclonal antibody in development for sars-cov-2 prophylaxis
topic Abstract
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10677384/
http://dx.doi.org/10.1093/ofid/ofad500.1185
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