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Enabling adoption of 2D-NMR for the higher order structure assessment of monoclonal antibody therapeutics

The increased interest in using monoclonal antibodies (mAbs) as a platform for biopharmaceuticals has led to the need for new analytical techniques that can precisely assess physicochemical properties of these large and very complex drugs for the purpose of correctly identifying quality attributes (...

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Autores principales: Brinson, Robert G., Marino, John P., Delaglio, Frank, Arbogast, Luke W., Evans, Ryan M., Kearsley, Anthony, Gingras, Geneviève, Ghasriani, Houman, Aubin, Yves, Pierens, Gregory K., Jia, Xinying, Mobli, Mehdi, Grant, Hamish G., Keizer, David W., Schweimer, Kristian, Ståhle, Jonas, Widmalm, Göran, Zartler, Edward R., Lawrence, Chad W., Reardon, Patrick N., Cort, John R., Xu, Ping, Ni, Feng, Yanaka, Saeko, Kato, Koichi, Parnham, Stuart R., Tsao, Desiree, Blomgren, Andreas, Rundlöf, Torgny, Trieloff, Nils, Schmieder, Peter, Ross, Alfred, Skidmore, Ken, Chen, Kang, Keire, David, Freedberg, Darón I., Suter-Stahel, Thea, Wider, Gerhard, Ilc, Gregor, Plavec, Janez, Bradley, Scott A., Baldisseri, Donna M., Sforça, Mauricio Luis, Zeri, Ana Carolina de Mattos, Wei, Julie Yu, Szabo, Christina M., Amezcua, Carlos A., Jordan, John B., Wikström, Mats
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Taylor & Francis 2018
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6343768/
https://www.ncbi.nlm.nih.gov/pubmed/30570405
http://dx.doi.org/10.1080/19420862.2018.1544454
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author Brinson, Robert G.
Marino, John P.
Delaglio, Frank
Arbogast, Luke W.
Evans, Ryan M.
Kearsley, Anthony
Gingras, Geneviève
Ghasriani, Houman
Aubin, Yves
Pierens, Gregory K.
Jia, Xinying
Mobli, Mehdi
Grant, Hamish G.
Keizer, David W.
Schweimer, Kristian
Ståhle, Jonas
Widmalm, Göran
Zartler, Edward R.
Lawrence, Chad W.
Reardon, Patrick N.
Cort, John R.
Xu, Ping
Ni, Feng
Yanaka, Saeko
Kato, Koichi
Parnham, Stuart R.
Tsao, Desiree
Blomgren, Andreas
Rundlöf, Torgny
Trieloff, Nils
Schmieder, Peter
Ross, Alfred
Skidmore, Ken
Chen, Kang
Keire, David
Freedberg, Darón I.
Suter-Stahel, Thea
Wider, Gerhard
Ilc, Gregor
Plavec, Janez
Bradley, Scott A.
Baldisseri, Donna M.
Sforça, Mauricio Luis
Zeri, Ana Carolina de Mattos
Wei, Julie Yu
Szabo, Christina M.
Amezcua, Carlos A.
Jordan, John B.
Wikström, Mats
author_facet Brinson, Robert G.
Marino, John P.
Delaglio, Frank
Arbogast, Luke W.
Evans, Ryan M.
Kearsley, Anthony
Gingras, Geneviève
Ghasriani, Houman
Aubin, Yves
Pierens, Gregory K.
Jia, Xinying
Mobli, Mehdi
Grant, Hamish G.
Keizer, David W.
Schweimer, Kristian
Ståhle, Jonas
Widmalm, Göran
Zartler, Edward R.
Lawrence, Chad W.
Reardon, Patrick N.
Cort, John R.
Xu, Ping
Ni, Feng
Yanaka, Saeko
Kato, Koichi
Parnham, Stuart R.
Tsao, Desiree
Blomgren, Andreas
Rundlöf, Torgny
Trieloff, Nils
Schmieder, Peter
Ross, Alfred
Skidmore, Ken
Chen, Kang
Keire, David
Freedberg, Darón I.
Suter-Stahel, Thea
Wider, Gerhard
Ilc, Gregor
Plavec, Janez
Bradley, Scott A.
Baldisseri, Donna M.
Sforça, Mauricio Luis
Zeri, Ana Carolina de Mattos
Wei, Julie Yu
Szabo, Christina M.
Amezcua, Carlos A.
Jordan, John B.
Wikström, Mats
author_sort Brinson, Robert G.
collection PubMed
description The increased interest in using monoclonal antibodies (mAbs) as a platform for biopharmaceuticals has led to the need for new analytical techniques that can precisely assess physicochemical properties of these large and very complex drugs for the purpose of correctly identifying quality attributes (QA). One QA, higher order structure (HOS), is unique to biopharmaceuticals and essential for establishing consistency in biopharmaceutical manufacturing, detecting process-related variations from manufacturing changes and establishing comparability between biologic products. To address this measurement challenge, two-dimensional nuclear magnetic resonance spectroscopy (2D-NMR) methods were introduced that allow for the precise atomic-level comparison of the HOS between two proteins, including mAbs. Here, an inter-laboratory comparison involving 26 industrial, government and academic laboratories worldwide was performed as a benchmark using the NISTmAb, from the National Institute of Standards and Technology (NIST), to facilitate the translation of the 2D-NMR method into routine use for biopharmaceutical product development. Two-dimensional (1)H,(15)N and (1)H,(13)C NMR spectra were acquired with harmonized experimental protocols on the unlabeled Fab domain and a uniformly enriched-(15)N, 20%-(13)C-enriched system suitability sample derived from the NISTmAb. Chemometric analyses from over 400 spectral maps acquired on 39 different NMR spectrometers ranging from 500 MHz to 900 MHz demonstrate spectral fingerprints that are fit-for-purpose for the assessment of HOS. The 2D-NMR method is shown to provide the measurement reliability needed to move the technique from an emerging technology to a harmonized, routine measurement that can be generally applied with great confidence to high precision assessments of the HOS of mAb-based biotherapeutics.
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spelling pubmed-63437682019-02-01 Enabling adoption of 2D-NMR for the higher order structure assessment of monoclonal antibody therapeutics Brinson, Robert G. Marino, John P. Delaglio, Frank Arbogast, Luke W. Evans, Ryan M. Kearsley, Anthony Gingras, Geneviève Ghasriani, Houman Aubin, Yves Pierens, Gregory K. Jia, Xinying Mobli, Mehdi Grant, Hamish G. Keizer, David W. Schweimer, Kristian Ståhle, Jonas Widmalm, Göran Zartler, Edward R. Lawrence, Chad W. Reardon, Patrick N. Cort, John R. Xu, Ping Ni, Feng Yanaka, Saeko Kato, Koichi Parnham, Stuart R. Tsao, Desiree Blomgren, Andreas Rundlöf, Torgny Trieloff, Nils Schmieder, Peter Ross, Alfred Skidmore, Ken Chen, Kang Keire, David Freedberg, Darón I. Suter-Stahel, Thea Wider, Gerhard Ilc, Gregor Plavec, Janez Bradley, Scott A. Baldisseri, Donna M. Sforça, Mauricio Luis Zeri, Ana Carolina de Mattos Wei, Julie Yu Szabo, Christina M. Amezcua, Carlos A. Jordan, John B. Wikström, Mats MAbs Report The increased interest in using monoclonal antibodies (mAbs) as a platform for biopharmaceuticals has led to the need for new analytical techniques that can precisely assess physicochemical properties of these large and very complex drugs for the purpose of correctly identifying quality attributes (QA). One QA, higher order structure (HOS), is unique to biopharmaceuticals and essential for establishing consistency in biopharmaceutical manufacturing, detecting process-related variations from manufacturing changes and establishing comparability between biologic products. To address this measurement challenge, two-dimensional nuclear magnetic resonance spectroscopy (2D-NMR) methods were introduced that allow for the precise atomic-level comparison of the HOS between two proteins, including mAbs. Here, an inter-laboratory comparison involving 26 industrial, government and academic laboratories worldwide was performed as a benchmark using the NISTmAb, from the National Institute of Standards and Technology (NIST), to facilitate the translation of the 2D-NMR method into routine use for biopharmaceutical product development. Two-dimensional (1)H,(15)N and (1)H,(13)C NMR spectra were acquired with harmonized experimental protocols on the unlabeled Fab domain and a uniformly enriched-(15)N, 20%-(13)C-enriched system suitability sample derived from the NISTmAb. Chemometric analyses from over 400 spectral maps acquired on 39 different NMR spectrometers ranging from 500 MHz to 900 MHz demonstrate spectral fingerprints that are fit-for-purpose for the assessment of HOS. The 2D-NMR method is shown to provide the measurement reliability needed to move the technique from an emerging technology to a harmonized, routine measurement that can be generally applied with great confidence to high precision assessments of the HOS of mAb-based biotherapeutics. Taylor & Francis 2018-12-22 /pmc/articles/PMC6343768/ /pubmed/30570405 http://dx.doi.org/10.1080/19420862.2018.1544454 Text en © 2018 The Author(s). Published with license by Taylor & Francis Group, LLC http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an Open Access article distributed under the terms of the Creative Commons Attribution-NonCommercial-NoDerivatives License (http://creativecommons.org/licenses/by-nc-nd/4.0/), which permits non-commercial re-use, distribution, and reproduction in any medium, provided the original work is properly cited, and is not altered, transformed, or built upon in any way.
spellingShingle Report
Brinson, Robert G.
Marino, John P.
Delaglio, Frank
Arbogast, Luke W.
Evans, Ryan M.
Kearsley, Anthony
Gingras, Geneviève
Ghasriani, Houman
Aubin, Yves
Pierens, Gregory K.
Jia, Xinying
Mobli, Mehdi
Grant, Hamish G.
Keizer, David W.
Schweimer, Kristian
Ståhle, Jonas
Widmalm, Göran
Zartler, Edward R.
Lawrence, Chad W.
Reardon, Patrick N.
Cort, John R.
Xu, Ping
Ni, Feng
Yanaka, Saeko
Kato, Koichi
Parnham, Stuart R.
Tsao, Desiree
Blomgren, Andreas
Rundlöf, Torgny
Trieloff, Nils
Schmieder, Peter
Ross, Alfred
Skidmore, Ken
Chen, Kang
Keire, David
Freedberg, Darón I.
Suter-Stahel, Thea
Wider, Gerhard
Ilc, Gregor
Plavec, Janez
Bradley, Scott A.
Baldisseri, Donna M.
Sforça, Mauricio Luis
Zeri, Ana Carolina de Mattos
Wei, Julie Yu
Szabo, Christina M.
Amezcua, Carlos A.
Jordan, John B.
Wikström, Mats
Enabling adoption of 2D-NMR for the higher order structure assessment of monoclonal antibody therapeutics
title Enabling adoption of 2D-NMR for the higher order structure assessment of monoclonal antibody therapeutics
title_full Enabling adoption of 2D-NMR for the higher order structure assessment of monoclonal antibody therapeutics
title_fullStr Enabling adoption of 2D-NMR for the higher order structure assessment of monoclonal antibody therapeutics
title_full_unstemmed Enabling adoption of 2D-NMR for the higher order structure assessment of monoclonal antibody therapeutics
title_short Enabling adoption of 2D-NMR for the higher order structure assessment of monoclonal antibody therapeutics
title_sort enabling adoption of 2d-nmr for the higher order structure assessment of monoclonal antibody therapeutics
topic Report
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6343768/
https://www.ncbi.nlm.nih.gov/pubmed/30570405
http://dx.doi.org/10.1080/19420862.2018.1544454
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