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Quantification of citrullinated histones: Development of an improved assay to reliably quantify nucleosomal H3Cit in human plasma

BACKGROUND: Recent data propose a diagnostic and prognostic capacity for citrullinated histone H3 (H3Cit), a marker of neutrophil extracellular traps (NETs), in pathologic conditions such as cancer and thrombosis. However, current research is hampered by lack of standardized assays. OBJECTIVES: We a...

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Autores principales: Thålin, Charlotte, Aguilera, Katherina, Hall, Nathan W., Marunde, Matthew R., Burg, Jonathan M., Rosell, Axel, Daleskog, Maud, Månsson, Maja, Hisada, Yohei, Meiners, Matthew J., Sun, Zu-Wen, Whelihan, Matthew F., Cheek, Marcus A., Howard, Sarah A., Saxena-Beem, Shruti, Noubouossie, Denis F., Key, Nigel S., Sheikh, Saira Z., Keogh, Michael-Christopher, Cowles, Martis W., Lundström, Staffan, Mackman, Nigel, Wallén, Håkan, Johnstone, Andrea L.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8722705/
https://www.ncbi.nlm.nih.gov/pubmed/32654410
http://dx.doi.org/10.1111/jth.15003
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author Thålin, Charlotte
Aguilera, Katherina
Hall, Nathan W.
Marunde, Matthew R.
Burg, Jonathan M.
Rosell, Axel
Daleskog, Maud
Månsson, Maja
Hisada, Yohei
Meiners, Matthew J.
Sun, Zu-Wen
Whelihan, Matthew F.
Cheek, Marcus A.
Howard, Sarah A.
Saxena-Beem, Shruti
Noubouossie, Denis F.
Key, Nigel S.
Sheikh, Saira Z.
Keogh, Michael-Christopher
Cowles, Martis W.
Lundström, Staffan
Mackman, Nigel
Wallén, Håkan
Johnstone, Andrea L.
author_facet Thålin, Charlotte
Aguilera, Katherina
Hall, Nathan W.
Marunde, Matthew R.
Burg, Jonathan M.
Rosell, Axel
Daleskog, Maud
Månsson, Maja
Hisada, Yohei
Meiners, Matthew J.
Sun, Zu-Wen
Whelihan, Matthew F.
Cheek, Marcus A.
Howard, Sarah A.
Saxena-Beem, Shruti
Noubouossie, Denis F.
Key, Nigel S.
Sheikh, Saira Z.
Keogh, Michael-Christopher
Cowles, Martis W.
Lundström, Staffan
Mackman, Nigel
Wallén, Håkan
Johnstone, Andrea L.
author_sort Thålin, Charlotte
collection PubMed
description BACKGROUND: Recent data propose a diagnostic and prognostic capacity for citrullinated histone H3 (H3Cit), a marker of neutrophil extracellular traps (NETs), in pathologic conditions such as cancer and thrombosis. However, current research is hampered by lack of standardized assays. OBJECTIVES: We aimed to develop an assay to reliably quantify nucleosomal H3Cit in human plasma. METHODS: We assessed the common practice of in vitro enzymatically modified histone H3 as calibration standards and the specificity of available intrapeptidyl citrulline antibodies. Based on our findings, we developed and validated a novel assay to quantify nucleosomal H3Cit in human plasma. RESULTS: We show that enzymatically citrullinated H3 proteins are compromised by high enzyme-dependent lot variability as well as instability in plasma. We furthermore demonstrate that the majority of commercially available antibodies against intrapeptidyl citrulline display poor specificity for their reported target when tested against a panel of semi-synthetic nucleosomes containing distinct histone H3 citrullinations. Finally, we present a novel assay utilizing highly specific monoclonal antibodies and semi-synthetic nucleosomes containing citrulline in place of arginine at histone H3, arginine residues 2, 8, and 17 (H3R2,8,17Cit) as calibration standards. Rigorous validation of this assay shows its capacity to accurately and reliably quantify nucleosomal H3Cit levels in human plasma with clear elevations in cancer patients compared to healthy individuals. CONCLUSIONS: Our novel approach using defined nucleosome controls enables reliable quantification of H3Cit in human plasma. This assay will be broadly applicable to study the role of histone citrullination in disease and its utility as a biomarker.
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spelling pubmed-87227052022-01-03 Quantification of citrullinated histones: Development of an improved assay to reliably quantify nucleosomal H3Cit in human plasma Thålin, Charlotte Aguilera, Katherina Hall, Nathan W. Marunde, Matthew R. Burg, Jonathan M. Rosell, Axel Daleskog, Maud Månsson, Maja Hisada, Yohei Meiners, Matthew J. Sun, Zu-Wen Whelihan, Matthew F. Cheek, Marcus A. Howard, Sarah A. Saxena-Beem, Shruti Noubouossie, Denis F. Key, Nigel S. Sheikh, Saira Z. Keogh, Michael-Christopher Cowles, Martis W. Lundström, Staffan Mackman, Nigel Wallén, Håkan Johnstone, Andrea L. J Thromb Haemost Article BACKGROUND: Recent data propose a diagnostic and prognostic capacity for citrullinated histone H3 (H3Cit), a marker of neutrophil extracellular traps (NETs), in pathologic conditions such as cancer and thrombosis. However, current research is hampered by lack of standardized assays. OBJECTIVES: We aimed to develop an assay to reliably quantify nucleosomal H3Cit in human plasma. METHODS: We assessed the common practice of in vitro enzymatically modified histone H3 as calibration standards and the specificity of available intrapeptidyl citrulline antibodies. Based on our findings, we developed and validated a novel assay to quantify nucleosomal H3Cit in human plasma. RESULTS: We show that enzymatically citrullinated H3 proteins are compromised by high enzyme-dependent lot variability as well as instability in plasma. We furthermore demonstrate that the majority of commercially available antibodies against intrapeptidyl citrulline display poor specificity for their reported target when tested against a panel of semi-synthetic nucleosomes containing distinct histone H3 citrullinations. Finally, we present a novel assay utilizing highly specific monoclonal antibodies and semi-synthetic nucleosomes containing citrulline in place of arginine at histone H3, arginine residues 2, 8, and 17 (H3R2,8,17Cit) as calibration standards. Rigorous validation of this assay shows its capacity to accurately and reliably quantify nucleosomal H3Cit levels in human plasma with clear elevations in cancer patients compared to healthy individuals. CONCLUSIONS: Our novel approach using defined nucleosome controls enables reliable quantification of H3Cit in human plasma. This assay will be broadly applicable to study the role of histone citrullination in disease and its utility as a biomarker. 2020-08-08 2020-10 /pmc/articles/PMC8722705/ /pubmed/32654410 http://dx.doi.org/10.1111/jth.15003 Text en https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the terms of the Creative Commons Attribution-NonCommercial-NoDerivs License, which permits use and distribution in any medium, provided the original work is properly cited, the use is non-commercial and no modifications or adaptations are made.
spellingShingle Article
Thålin, Charlotte
Aguilera, Katherina
Hall, Nathan W.
Marunde, Matthew R.
Burg, Jonathan M.
Rosell, Axel
Daleskog, Maud
Månsson, Maja
Hisada, Yohei
Meiners, Matthew J.
Sun, Zu-Wen
Whelihan, Matthew F.
Cheek, Marcus A.
Howard, Sarah A.
Saxena-Beem, Shruti
Noubouossie, Denis F.
Key, Nigel S.
Sheikh, Saira Z.
Keogh, Michael-Christopher
Cowles, Martis W.
Lundström, Staffan
Mackman, Nigel
Wallén, Håkan
Johnstone, Andrea L.
Quantification of citrullinated histones: Development of an improved assay to reliably quantify nucleosomal H3Cit in human plasma
title Quantification of citrullinated histones: Development of an improved assay to reliably quantify nucleosomal H3Cit in human plasma
title_full Quantification of citrullinated histones: Development of an improved assay to reliably quantify nucleosomal H3Cit in human plasma
title_fullStr Quantification of citrullinated histones: Development of an improved assay to reliably quantify nucleosomal H3Cit in human plasma
title_full_unstemmed Quantification of citrullinated histones: Development of an improved assay to reliably quantify nucleosomal H3Cit in human plasma
title_short Quantification of citrullinated histones: Development of an improved assay to reliably quantify nucleosomal H3Cit in human plasma
title_sort quantification of citrullinated histones: development of an improved assay to reliably quantify nucleosomal h3cit in human plasma
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8722705/
https://www.ncbi.nlm.nih.gov/pubmed/32654410
http://dx.doi.org/10.1111/jth.15003
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