Prediction of the binding interface between monoclonal antibody m102.4 and Nipah attachment glycoprotein using structure-guided alanine scanning and computational docking

Nipah Virus (NiV) has been designated as a priority disease with an urgent need for therapeutic development by World Health Organization. The monoclonal antibody m102.4 binds to the immunodominant NiV receptor-binding glycoprotein (GP), and potently neutralizes NiV, indicating its potential as a the...

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Autores principales: Tit-oon, Phanthakarn, Tharakaraman, Kannan, Artpradit, Charlermchai, Godavarthi, Abhinav, Sungkeeree, Pareenart, Sasisekharan, Varun, Kerdwong, Jarunee, Miller, Nathaniel Loren, Mahajan, Bhuvna, Khongmanee, Amnart, Ruchirawat, Mathuros, Sasisekharan, Ram, Fuangthong, Mayuree
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Nature Publishing Group UK 2020
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7588459/
https://www.ncbi.nlm.nih.gov/pubmed/33106487
http://dx.doi.org/10.1038/s41598-020-75056-y
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author Tit-oon, Phanthakarn
Tharakaraman, Kannan
Artpradit, Charlermchai
Godavarthi, Abhinav
Sungkeeree, Pareenart
Sasisekharan, Varun
Kerdwong, Jarunee
Miller, Nathaniel Loren
Mahajan, Bhuvna
Khongmanee, Amnart
Ruchirawat, Mathuros
Sasisekharan, Ram
Fuangthong, Mayuree
author_facet Tit-oon, Phanthakarn
Tharakaraman, Kannan
Artpradit, Charlermchai
Godavarthi, Abhinav
Sungkeeree, Pareenart
Sasisekharan, Varun
Kerdwong, Jarunee
Miller, Nathaniel Loren
Mahajan, Bhuvna
Khongmanee, Amnart
Ruchirawat, Mathuros
Sasisekharan, Ram
Fuangthong, Mayuree
author_sort Tit-oon, Phanthakarn
collection PubMed
description Nipah Virus (NiV) has been designated as a priority disease with an urgent need for therapeutic development by World Health Organization. The monoclonal antibody m102.4 binds to the immunodominant NiV receptor-binding glycoprotein (GP), and potently neutralizes NiV, indicating its potential as a therapeutic agent. Although the co-crystal structure of m102.3, an m102.4 derivative, in complex with the GP of the related Hendra Virus (HeV) has been solved, the structural interaction between m102.4 and NiV is uncharacterized. Herein, we used structure-guided alanine-scanning mutagenesis to map the functional epitope and paratope residues that govern the antigen–antibody interaction. Our results revealed that the binding of m102.4 is mediated predominantly by two residues in the HCDR3 region, which is unusually small for an antibody-antigen interaction. We performed computational docking to generate a structural model of m102.4-NiV interaction. Our model indicates that m102.4 targets the common hydrophobic central cavity and a hydrophilic rim on the GP, as observed for the m102.3-HeV co-crystal, albeit with Fv orientation differences. In summary, our study provides insight into the m102.4-NiV interaction, demonstrating that structure-guided alanine-scanning and computational modeling can serve as the starting point for additional antibody reengineering (e.g. affinity maturation) to generate potential therapeutic candidates.
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spelling pubmed-75884592020-10-27 Prediction of the binding interface between monoclonal antibody m102.4 and Nipah attachment glycoprotein using structure-guided alanine scanning and computational docking Tit-oon, Phanthakarn Tharakaraman, Kannan Artpradit, Charlermchai Godavarthi, Abhinav Sungkeeree, Pareenart Sasisekharan, Varun Kerdwong, Jarunee Miller, Nathaniel Loren Mahajan, Bhuvna Khongmanee, Amnart Ruchirawat, Mathuros Sasisekharan, Ram Fuangthong, Mayuree Sci Rep Article Nipah Virus (NiV) has been designated as a priority disease with an urgent need for therapeutic development by World Health Organization. The monoclonal antibody m102.4 binds to the immunodominant NiV receptor-binding glycoprotein (GP), and potently neutralizes NiV, indicating its potential as a therapeutic agent. Although the co-crystal structure of m102.3, an m102.4 derivative, in complex with the GP of the related Hendra Virus (HeV) has been solved, the structural interaction between m102.4 and NiV is uncharacterized. Herein, we used structure-guided alanine-scanning mutagenesis to map the functional epitope and paratope residues that govern the antigen–antibody interaction. Our results revealed that the binding of m102.4 is mediated predominantly by two residues in the HCDR3 region, which is unusually small for an antibody-antigen interaction. We performed computational docking to generate a structural model of m102.4-NiV interaction. Our model indicates that m102.4 targets the common hydrophobic central cavity and a hydrophilic rim on the GP, as observed for the m102.3-HeV co-crystal, albeit with Fv orientation differences. In summary, our study provides insight into the m102.4-NiV interaction, demonstrating that structure-guided alanine-scanning and computational modeling can serve as the starting point for additional antibody reengineering (e.g. affinity maturation) to generate potential therapeutic candidates. Nature Publishing Group UK 2020-10-26 /pmc/articles/PMC7588459/ /pubmed/33106487 http://dx.doi.org/10.1038/s41598-020-75056-y Text en © The Author(s) 2020 Open Access This article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons licence, and indicate if changes were made. The images or other third party material in this article are included in the article's Creative Commons licence, unless indicated otherwise in a credit line to the material. If material is not included in the article's Creative Commons licence and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this licence, visit http://creativecommons.org/licenses/by/4.0/.
spellingShingle Article
Tit-oon, Phanthakarn
Tharakaraman, Kannan
Artpradit, Charlermchai
Godavarthi, Abhinav
Sungkeeree, Pareenart
Sasisekharan, Varun
Kerdwong, Jarunee
Miller, Nathaniel Loren
Mahajan, Bhuvna
Khongmanee, Amnart
Ruchirawat, Mathuros
Sasisekharan, Ram
Fuangthong, Mayuree
Prediction of the binding interface between monoclonal antibody m102.4 and Nipah attachment glycoprotein using structure-guided alanine scanning and computational docking
title Prediction of the binding interface between monoclonal antibody m102.4 and Nipah attachment glycoprotein using structure-guided alanine scanning and computational docking
title_full Prediction of the binding interface between monoclonal antibody m102.4 and Nipah attachment glycoprotein using structure-guided alanine scanning and computational docking
title_fullStr Prediction of the binding interface between monoclonal antibody m102.4 and Nipah attachment glycoprotein using structure-guided alanine scanning and computational docking
title_full_unstemmed Prediction of the binding interface between monoclonal antibody m102.4 and Nipah attachment glycoprotein using structure-guided alanine scanning and computational docking
title_short Prediction of the binding interface between monoclonal antibody m102.4 and Nipah attachment glycoprotein using structure-guided alanine scanning and computational docking
title_sort prediction of the binding interface between monoclonal antibody m102.4 and nipah attachment glycoprotein using structure-guided alanine scanning and computational docking
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7588459/
https://www.ncbi.nlm.nih.gov/pubmed/33106487
http://dx.doi.org/10.1038/s41598-020-75056-y
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