Multicenter Longitudinal Quality Assessment of MS-Based Proteomics in Plasma and Serum

Oliver Kardell; Thomas Gronauer; Christine von Toerne; Juliane Merl-Pham; Ann Christine König; Teresa K. Barth; Julia Mergner; Christina Ludwig; Johanna Tüshaus; Pieter Giesbertz; Stephan Breimann; Lisa Schweizer; Torsten Müller; Georg Kliewer; Ute Distler; David Gomez-Zepeda; Oliver Popp; Di Qin; Daniel Teupser; Jürgen Cox; Axel Imhof; Bernhard Küster; Stefan F. Lichtenthaler; Jeroen Krijgsveld; Stefan Tenzer; Philipp Mertins; Fabian Coscia; Stefanie M. Hauck

doi:10.1021/acs.jproteome.4c00644

Multicenter Longitudinal Quality Assessment of MS-Based Proteomics in Plasma and Serum

Oliver Kardell, Thomas Gronauer, Christine von Toerne, Juliane Merl-Pham, Ann Christine König, Teresa K. Barth, Julia Mergner, Christina Ludwig, Johanna Tüshaus, Pieter Giesbertz, Stephan Breimann, Lisa Schweizer, Torsten Müller, Georg Kliewer, Ute Distler, David Gomez-Zepeda, Oliver Popp, Di Qin, Daniel Teupser, Jürgen CoxAxel Imhof, Bernhard Küster, Stefan F. Lichtenthaler, Jeroen Krijgsveld, Stefan Tenzer, Philipp Mertins, Fabian Coscia, Stefanie M. Hauck

Research output: Contribution to journal › Article › peer-review

Abstract

Advancing MS-based proteomics toward clinical applications evolves around developing standardized start-to-finish and fit-for-purpose workflows for clinical specimens. Steps along the method design involve the determination and optimization of several bioanalytical parameters such as selectivity, sensitivity, accuracy, and precision. In a joint effort, eight proteomics laboratories belonging to the MSCoreSys initiative including the CLINSPECT-M, MSTARS, DIASyM, and SMART-CARE consortia performed a longitudinal round-robin study to assess the analysis performance of plasma and serum as clinically relevant samples. A variety of LC-MS/MS setups including mass spectrometer models from ThermoFisher and Bruker as well as LC systems from ThermoFisher, Evosep, and Waters Corporation were used in this study. As key performance indicators, sensitivity, precision, and reproducibility were monitored over time. Protein identifications range between 300 and 400 IDs across different state-of-the-art MS instruments, with timsTOF Pro, Orbitrap Exploris 480, and Q Exactive HF-X being among the top performers. Overall, 71 proteins are reproducibly detectable in all setups in both serum and plasma samples, and 22 of these proteins are FDA-approved biomarkers, which are reproducibly quantified (CV < 20% with label-free quantification). In total, the round-robin study highlights a promising baseline for bringing MS-based measurements of serum and plasma samples closer to clinical utility.

Original language	English
Pages (from-to)	1017-1029
Number of pages	13
Journal	Journal of Proteome Research
Volume	24
Issue number	3
DOIs	https://doi.org/10.1021/acs.jproteome.4c00644
State	Published - 7 Mar 2025

Keywords

LC-MS/MS
R package mpwR
clinical specimen
longitudinal round-robin study
plasma
serum

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10.1021/acs.jproteome.4c00644

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Kardell, O., Gronauer, T., von Toerne, C., Merl-Pham, J., König, A. C., Barth, T. K., Mergner, J., Ludwig, C., Tüshaus, J., Giesbertz, P., Breimann, S., Schweizer, L., Müller, T., Kliewer, G., Distler, U., Gomez-Zepeda, D., Popp, O., Qin, D., Teupser, D., ... Hauck, S. M. (2025). Multicenter Longitudinal Quality Assessment of MS-Based Proteomics in Plasma and Serum. Journal of Proteome Research, 24(3), 1017-1029. https://doi.org/10.1021/acs.jproteome.4c00644

@article{2126d682695d474a9e9e8f2a016fa3cf,

title = "Multicenter Longitudinal Quality Assessment of MS-Based Proteomics in Plasma and Serum",

abstract = "Advancing MS-based proteomics toward clinical applications evolves around developing standardized start-to-finish and fit-for-purpose workflows for clinical specimens. Steps along the method design involve the determination and optimization of several bioanalytical parameters such as selectivity, sensitivity, accuracy, and precision. In a joint effort, eight proteomics laboratories belonging to the MSCoreSys initiative including the CLINSPECT-M, MSTARS, DIASyM, and SMART-CARE consortia performed a longitudinal round-robin study to assess the analysis performance of plasma and serum as clinically relevant samples. A variety of LC-MS/MS setups including mass spectrometer models from ThermoFisher and Bruker as well as LC systems from ThermoFisher, Evosep, and Waters Corporation were used in this study. As key performance indicators, sensitivity, precision, and reproducibility were monitored over time. Protein identifications range between 300 and 400 IDs across different state-of-the-art MS instruments, with timsTOF Pro, Orbitrap Exploris 480, and Q Exactive HF-X being among the top performers. Overall, 71 proteins are reproducibly detectable in all setups in both serum and plasma samples, and 22 of these proteins are FDA-approved biomarkers, which are reproducibly quantified (CV < 20% with label-free quantification). In total, the round-robin study highlights a promising baseline for bringing MS-based measurements of serum and plasma samples closer to clinical utility.",

keywords = "LC-MS/MS, R package mpwR, clinical specimen, longitudinal round-robin study, plasma, serum",

author = "Oliver Kardell and Thomas Gronauer and {von Toerne}, Christine and Juliane Merl-Pham and K{\"o}nig, {Ann Christine} and Barth, {Teresa K.} and Julia Mergner and Christina Ludwig and Johanna T{\"u}shaus and Pieter Giesbertz and Stephan Breimann and Lisa Schweizer and Torsten M{\"u}ller and Georg Kliewer and Ute Distler and David Gomez-Zepeda and Oliver Popp and Di Qin and Daniel Teupser and J{\"u}rgen Cox and Axel Imhof and Bernhard K{\"u}ster and Lichtenthaler, {Stefan F.} and Jeroen Krijgsveld and Stefan Tenzer and Philipp Mertins and Fabian Coscia and Hauck, {Stefanie M.}",

note = "Publisher Copyright: {\textcopyright} 2025 The Authors. Published by American Chemical Society.",

year = "2025",

month = mar,

day = "7",

doi = "10.1021/acs.jproteome.4c00644",

language = "English",

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Kardell, O, Gronauer, T, von Toerne, C, Merl-Pham, J, König, AC, Barth, TK, Mergner, J, Ludwig, C, Tüshaus, J, Giesbertz, P, Breimann, S, Schweizer, L, Müller, T, Kliewer, G, Distler, U, Gomez-Zepeda, D, Popp, O, Qin, D, Teupser, D, Cox, J, Imhof, A, Küster, B , Lichtenthaler, SF, Krijgsveld, J, Tenzer, S, Mertins, P, Coscia, F & Hauck, SM 2025, 'Multicenter Longitudinal Quality Assessment of MS-Based Proteomics in Plasma and Serum', Journal of Proteome Research, vol. 24, no. 3, pp. 1017-1029. https://doi.org/10.1021/acs.jproteome.4c00644

TY - JOUR

T1 - Multicenter Longitudinal Quality Assessment of MS-Based Proteomics in Plasma and Serum

AU - Kardell, Oliver

AU - Gronauer, Thomas

AU - von Toerne, Christine

AU - Merl-Pham, Juliane

AU - König, Ann Christine

AU - Barth, Teresa K.

AU - Mergner, Julia

AU - Ludwig, Christina

AU - Tüshaus, Johanna

AU - Giesbertz, Pieter

AU - Breimann, Stephan

AU - Schweizer, Lisa

AU - Müller, Torsten

AU - Kliewer, Georg

AU - Distler, Ute

AU - Gomez-Zepeda, David

AU - Popp, Oliver

AU - Qin, Di

AU - Teupser, Daniel

AU - Cox, Jürgen

AU - Imhof, Axel

AU - Küster, Bernhard

AU - Lichtenthaler, Stefan F.

AU - Krijgsveld, Jeroen

AU - Tenzer, Stefan

AU - Mertins, Philipp

AU - Coscia, Fabian

AU - Hauck, Stefanie M.

PY - 2025/3/7

Y1 - 2025/3/7

N2 - Advancing MS-based proteomics toward clinical applications evolves around developing standardized start-to-finish and fit-for-purpose workflows for clinical specimens. Steps along the method design involve the determination and optimization of several bioanalytical parameters such as selectivity, sensitivity, accuracy, and precision. In a joint effort, eight proteomics laboratories belonging to the MSCoreSys initiative including the CLINSPECT-M, MSTARS, DIASyM, and SMART-CARE consortia performed a longitudinal round-robin study to assess the analysis performance of plasma and serum as clinically relevant samples. A variety of LC-MS/MS setups including mass spectrometer models from ThermoFisher and Bruker as well as LC systems from ThermoFisher, Evosep, and Waters Corporation were used in this study. As key performance indicators, sensitivity, precision, and reproducibility were monitored over time. Protein identifications range between 300 and 400 IDs across different state-of-the-art MS instruments, with timsTOF Pro, Orbitrap Exploris 480, and Q Exactive HF-X being among the top performers. Overall, 71 proteins are reproducibly detectable in all setups in both serum and plasma samples, and 22 of these proteins are FDA-approved biomarkers, which are reproducibly quantified (CV < 20% with label-free quantification). In total, the round-robin study highlights a promising baseline for bringing MS-based measurements of serum and plasma samples closer to clinical utility.

AB - Advancing MS-based proteomics toward clinical applications evolves around developing standardized start-to-finish and fit-for-purpose workflows for clinical specimens. Steps along the method design involve the determination and optimization of several bioanalytical parameters such as selectivity, sensitivity, accuracy, and precision. In a joint effort, eight proteomics laboratories belonging to the MSCoreSys initiative including the CLINSPECT-M, MSTARS, DIASyM, and SMART-CARE consortia performed a longitudinal round-robin study to assess the analysis performance of plasma and serum as clinically relevant samples. A variety of LC-MS/MS setups including mass spectrometer models from ThermoFisher and Bruker as well as LC systems from ThermoFisher, Evosep, and Waters Corporation were used in this study. As key performance indicators, sensitivity, precision, and reproducibility were monitored over time. Protein identifications range between 300 and 400 IDs across different state-of-the-art MS instruments, with timsTOF Pro, Orbitrap Exploris 480, and Q Exactive HF-X being among the top performers. Overall, 71 proteins are reproducibly detectable in all setups in both serum and plasma samples, and 22 of these proteins are FDA-approved biomarkers, which are reproducibly quantified (CV < 20% with label-free quantification). In total, the round-robin study highlights a promising baseline for bringing MS-based measurements of serum and plasma samples closer to clinical utility.

KW - LC-MS/MS

KW - R package mpwR

KW - clinical specimen

KW - longitudinal round-robin study

KW - plasma

KW - serum

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U2 - 10.1021/acs.jproteome.4c00644

DO - 10.1021/acs.jproteome.4c00644

M3 - Article

AN - SCOPUS:85217260781

SN - 1535-3893

VL - 24

SP - 1017

EP - 1029

JO - Journal of Proteome Research

JF - Journal of Proteome Research

IS - 3

ER -

Multicenter Longitudinal Quality Assessment of MS-Based Proteomics in Plasma and Serum

Abstract

Keywords

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