Impact of infection on proteome-wide glycosylation revealed by distinct signatures for bacterial and viral pathogens

doi:10.1016/j.isci.2023.107257

Impact of infection on proteome-wide glycosylation revealed by distinct signatures for bacterial and viral pathogens

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Abstract

Mechanisms of infection and pathogenesis have predominantly been studied based on differential gene or protein expression. Less is known about posttranslational modifications, which are essential for protein functional diversity. We applied an innovative glycoproteomics method to study the systemic proteome-wide glycosylation in response to infection. The protein site-specific glycosylation was characterized in plasma derived from well-defined controls and patients. We found 3862 unique features, of which we identified 463 distinct intact glycopeptides, that could be mapped to more than 30 different proteins. Statistical analyses were used to derive a glycopeptide signature that enabled significant differentiation between patients with a bacterial or viral infection. Furthermore, supported by a machine learning algorithm, we demonstrated the ability to identify the causative pathogens based on the distinctive host blood plasma glycopeptide signatures. These results illustrate that glycoproteomics holds enormous potential as an innovative approach to improve the interpretation of relevant biological changes in response to infection.

Original language	English
Article number	107257
Pages (from-to)	1-18
Journal	iScience
Volume	26
Issue number	8
DOIs	https://doi.org/10.1016/j.isci.2023.107257
Publication status	Published - 18 Aug 2023

Keywords

Glycobiology
Glycomics
Health sciences
Immunology

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10.1016/j.isci.2023.107257Licence: CC BY-NC-ND

1-s2.0-S2589004223013342-mainFinal published version, 4.99 MBLicence: CC BY-NC-ND

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@article{7ca8c9ba9db44a60867718fdbf979b51,

title = "Impact of infection on proteome-wide glycosylation revealed by distinct signatures for bacterial and viral pathogens",

abstract = "Mechanisms of infection and pathogenesis have predominantly been studied based on differential gene or protein expression. Less is known about posttranslational modifications, which are essential for protein functional diversity. We applied an innovative glycoproteomics method to study the systemic proteome-wide glycosylation in response to infection. The protein site-specific glycosylation was characterized in plasma derived from well-defined controls and patients. We found 3862 unique features, of which we identified 463 distinct intact glycopeptides, that could be mapped to more than 30 different proteins. Statistical analyses were used to derive a glycopeptide signature that enabled significant differentiation between patients with a bacterial or viral infection. Furthermore, supported by a machine learning algorithm, we demonstrated the ability to identify the causative pathogens based on the distinctive host blood plasma glycopeptide signatures. These results illustrate that glycoproteomics holds enormous potential as an innovative approach to improve the interpretation of relevant biological changes in response to infection.",

keywords = "Glycobiology, Glycomics, Health sciences, Immunology",

author = "Esther Willems and Jolein Gloerich and Anouk Suppers and \{van der Flier\}, Michiel and \{van den Heuvel\}, \{Lambert P.\} and \{van de Kar\}, Nicole and Philipsen, \{Ria H.L.A.\} and \{van Dael\}, Maurice and Myrsini Kaforou and Wright, \{Victoria J.\} and Herberg, \{Jethro A.\} and Torres, \{Federico Martinon\} and Michael Levin and \{de Groot\}, Ronald and \{van Gool\}, \{Alain J.\} and Lefeber, \{Dirk J.\} and Wessels, \{Hans J.C.T.\} and \{de Jonge\}, \{Marien I.\} and Amina Abdulla and Christoph Aebi and \{van Aerde\}, Koen and Rachel Agbeko and Philipp Agyeman and Umberto D'alessandro and Ladan Ali and Wynand Alkema and Karen Allen and Gonz{\'a}lez, \{Fernando {\'A}lvez\} and Suzanne Anderson and Imran Ansari and Tasnim Araf and Tanja Avramoska and Bryan Baas and Natalija Bahovec and Farto, \{Cristina Balo\} and Anda Balode and Barendregt, \{A. M.\} and Ruth Barral-Arca and Castro, \{Mar{\'i}a Barreiro\} and Arta Bārzdiņa and David Bath and Sebastian Bauchinger and Lucas Baumard and Hinrich Baumgart and \{van den Berg\}, \{J. M.\} and J. Heidema and Ilse Jongerius and Miedema, \{C. J.\} and D. Schonenberg and Judith Zandstra",

note = "Funding Information: This research, part of the PERFORM project, has received funding from the European Union{\textquoteright}s Horizon 2020 research and innovation program under grant agreement No. 668303 . The samples collected previously were funded by: the European Seventh Framework Programme for Research and Technological Development ( FP7 ) under EUCLIDS Grant Agreement No. 279185 . Funding Information: This research, part of the PERFORM project, has received funding from the European Union's Horizon 2020 research and innovation program under grant agreement No. 668303. The samples collected previously were funded by: the European Seventh Framework Programme for Research and Technological Development (FP7) under EUCLIDS Grant Agreement No. 279185. We would like to thank all the patients and the healthy controls for donating their blood for the EUCLIDS, IRIS, and Westra studies. We would like to thank the Radboud Consortium for Glycoscience for their advice for data interpretation. We also thank the PERFORM consortium (see supplemental material for all participants) for their collaboration and fruitful discussions. Conceptualization, E.W. H.W. and M.J.; Methodology, E.W. M.D. H.W. and M.J.; Investigation, E.W.; Software, A.S. and H.W.; Formal Analysis, E.W. and H.W.; Visualization, E.W. and H.W.; Resources, M.F. L.H. N.K. R.P. M.K. V.W. J.H. and F.M.; Writing – Original Draft, E.W. and M.J.; Writing – Review \& Editing, E.W. J.G. A.S. M.F. L.H. N.K. R.P. M.D. M.K. V.W. J.H. F.M. M.L. R.G. A.G. D.L. H.W. and M.J.; Funding Acquisition, M.J. R.G. and M.L.; Supervision, H.W. D.L. and M.J. The authors declare no competing interests. We support inclusive, diverse, and equitable conduct of research. Publisher Copyright: {\textcopyright} 2023 The Author(s)",

year = "2023",

month = aug,

day = "18",

doi = "10.1016/j.isci.2023.107257",

language = "English",

volume = "26",

pages = "1--18",

journal = "iScience",

publisher = "Elsevier",

number = "8",

}

TY - JOUR

T1 - Impact of infection on proteome-wide glycosylation revealed by distinct signatures for bacterial and viral pathogens

AU - Willems, Esther

AU - Gloerich, Jolein

AU - Suppers, Anouk

AU - van der Flier, Michiel

AU - van den Heuvel, Lambert P.

AU - van de Kar, Nicole

AU - Philipsen, Ria H.L.A.

AU - van Dael, Maurice

AU - Kaforou, Myrsini

AU - Wright, Victoria J.

AU - Herberg, Jethro A.

AU - Torres, Federico Martinon

AU - Levin, Michael

AU - de Groot, Ronald

AU - van Gool, Alain J.

AU - Lefeber, Dirk J.

AU - Wessels, Hans J.C.T.

AU - de Jonge, Marien I.

AU - Abdulla, Amina

AU - Aebi, Christoph

AU - van Aerde, Koen

AU - Agbeko, Rachel

AU - Agyeman, Philipp

AU - D'alessandro, Umberto

AU - Ali, Ladan

AU - Alkema, Wynand

AU - Allen, Karen

AU - González, Fernando Álvez

AU - Anderson, Suzanne

AU - Ansari, Imran

AU - Araf, Tasnim

AU - Avramoska, Tanja

AU - Baas, Bryan

AU - Bahovec, Natalija

AU - Farto, Cristina Balo

AU - Balode, Anda

AU - Barendregt, A. M.

AU - Barral-Arca, Ruth

AU - Castro, María Barreiro

AU - Bārzdiņa, Arta

AU - Bath, David

AU - Bauchinger, Sebastian

AU - Baumard, Lucas

AU - Baumgart, Hinrich

AU - van den Berg, J. M.

AU - Heidema, J.

AU - Jongerius, Ilse

AU - Miedema, C. J.

AU - Schonenberg, D.

AU - Zandstra, Judith

N1 - Funding Information: This research, part of the PERFORM project, has received funding from the European Union’s Horizon 2020 research and innovation program under grant agreement No. 668303 . The samples collected previously were funded by: the European Seventh Framework Programme for Research and Technological Development ( FP7 ) under EUCLIDS Grant Agreement No. 279185 . Funding Information: This research, part of the PERFORM project, has received funding from the European Union's Horizon 2020 research and innovation program under grant agreement No. 668303. The samples collected previously were funded by: the European Seventh Framework Programme for Research and Technological Development (FP7) under EUCLIDS Grant Agreement No. 279185. We would like to thank all the patients and the healthy controls for donating their blood for the EUCLIDS, IRIS, and Westra studies. We would like to thank the Radboud Consortium for Glycoscience for their advice for data interpretation. We also thank the PERFORM consortium (see supplemental material for all participants) for their collaboration and fruitful discussions. Conceptualization, E.W. H.W. and M.J.; Methodology, E.W. M.D. H.W. and M.J.; Investigation, E.W.; Software, A.S. and H.W.; Formal Analysis, E.W. and H.W.; Visualization, E.W. and H.W.; Resources, M.F. L.H. N.K. R.P. M.K. V.W. J.H. and F.M.; Writing – Original Draft, E.W. and M.J.; Writing – Review & Editing, E.W. J.G. A.S. M.F. L.H. N.K. R.P. M.D. M.K. V.W. J.H. F.M. M.L. R.G. A.G. D.L. H.W. and M.J.; Funding Acquisition, M.J. R.G. and M.L.; Supervision, H.W. D.L. and M.J. The authors declare no competing interests. We support inclusive, diverse, and equitable conduct of research. Publisher Copyright: © 2023 The Author(s)

PY - 2023/8/18

Y1 - 2023/8/18

N2 - Mechanisms of infection and pathogenesis have predominantly been studied based on differential gene or protein expression. Less is known about posttranslational modifications, which are essential for protein functional diversity. We applied an innovative glycoproteomics method to study the systemic proteome-wide glycosylation in response to infection. The protein site-specific glycosylation was characterized in plasma derived from well-defined controls and patients. We found 3862 unique features, of which we identified 463 distinct intact glycopeptides, that could be mapped to more than 30 different proteins. Statistical analyses were used to derive a glycopeptide signature that enabled significant differentiation between patients with a bacterial or viral infection. Furthermore, supported by a machine learning algorithm, we demonstrated the ability to identify the causative pathogens based on the distinctive host blood plasma glycopeptide signatures. These results illustrate that glycoproteomics holds enormous potential as an innovative approach to improve the interpretation of relevant biological changes in response to infection.

AB - Mechanisms of infection and pathogenesis have predominantly been studied based on differential gene or protein expression. Less is known about posttranslational modifications, which are essential for protein functional diversity. We applied an innovative glycoproteomics method to study the systemic proteome-wide glycosylation in response to infection. The protein site-specific glycosylation was characterized in plasma derived from well-defined controls and patients. We found 3862 unique features, of which we identified 463 distinct intact glycopeptides, that could be mapped to more than 30 different proteins. Statistical analyses were used to derive a glycopeptide signature that enabled significant differentiation between patients with a bacterial or viral infection. Furthermore, supported by a machine learning algorithm, we demonstrated the ability to identify the causative pathogens based on the distinctive host blood plasma glycopeptide signatures. These results illustrate that glycoproteomics holds enormous potential as an innovative approach to improve the interpretation of relevant biological changes in response to infection.

KW - Glycobiology

KW - Glycomics

KW - Health sciences

KW - Immunology

UR - https://www.scopus.com/pages/publications/85165028111

U2 - 10.1016/j.isci.2023.107257

DO - 10.1016/j.isci.2023.107257

M3 - Article

C2 - 37520696

AN - SCOPUS:85165028111

VL - 26

SP - 1

EP - 18

JO - iScience

JF - iScience

IS - 8

M1 - 107257

ER -

Impact of infection on proteome-wide glycosylation revealed by distinct signatures for bacterial and viral pathogens

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Keywords

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