Capillary electrophoresis-Mass spectrometry at Trial by Metabo-ring: Effective electrophoretic mobility for Reproducible and Robust Compound Annotation

Nicolas Drouin; Marlien Van Mever; Elena Tobolkina; Sabrina Ferre; Anne-Catherine Servais; Marie-Jia Gou; Laurent Nyssen; Marianne Fillet; Guinevere S M Lageveen-Kammeijer; Jan Nouta; Andrew J Chetwynd; Iseult Lynch; James A Thorn; Jens Meixner; Christopher Loessner; Myriam Taverna; Sylvie Liu; N Thuy Tran; Yannis Nicolas Francois; Antony Lechner; Reine Nehmé; Ghassan Al Hamoui Dit Banni; Rouba Nasreddine; Cyril Colas; Herbert H Lindner; Klaus Faserl; Christian Neusüß; Manuel Nelke; Stefan Laemmerer; Catherine Perrin; Claudia Bich; Coral Barbas; Ángeles López-Gonzálvez; Andras Guttman; Marton Szigeti; Philip Britz-McKibbin; Zachary Kroezen; Meera Shanmuganathan; Peter Nemes; Erika P Portero; Thomas Hankemeier; Santiago Codesido; Víctor González-Ruiz; Serge Rudaz; Rawi Ramautar

doi:10.1021/acs.analchem.0c03129

Capillary electrophoresis-Mass spectrometry at Trial by Metabo-ring: Effective electrophoretic mobility for Reproducible and Robust Compound Annotation

Nicolas Drouin, Marlien Van Mever, Elena Tobolkina, Sabrina Ferre, Anne-Catherine Servais, Marie-Jia Gou, Laurent Nyssen, Marianne Fillet, Guinevere S M Lageveen-Kammeijer, Jan Nouta, Andrew J Chetwynd, Iseult Lynch, James A Thorn, Jens Meixner, Christopher Loessner, Myriam Taverna, Sylvie Liu, N Thuy Tran, Yannis Nicolas Francois, Antony LechnerReine Nehmé, Ghassan Al Hamoui Dit Banni, Rouba Nasreddine, Cyril Colas, Herbert H Lindner, Klaus Faserl, Christian Neusüß, Manuel Nelke, Stefan Laemmerer, Catherine Perrin, Claudia Bich, Coral Barbas, Ángeles López-Gonzálvez, Andras Guttman, Marton Szigeti, Philip Britz-McKibbin, Zachary Kroezen, Meera Shanmuganathan, Peter Nemes, Erika P Portero, Thomas Hankemeier, Santiago Codesido, Víctor González-Ruiz, Serge Rudaz, Rawi Ramautar

Earth and Environmental Sciences

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

6 Citations (Scopus)

Abstract

Capillary zone electrophoresis-mass spectrometry (CE-MS) is a mature analytical tool for the efficient profiling of (highly) polar and ionizable compounds. However, the use of CE-MS in comparison to other separation techniques remains underrepresented in metabolomics, as this analytical approach is still perceived as technically challenging and less reproducible, notably for migration time. The latter is key for a reliable comparison of metabolic profiles and for unknown biomarker identification that is complementary to high resolution MS/MS. In this work, we present the results of a Metabo-ring trial involving 16 CE-MS platforms among 13 different laboratories spanning two continents. The goal was to assess the reproducibility and identification capability of CE-MS by employing effective electrophoretic mobility (μ eff) as the key parameter in comparison to the relative migration time (RMT) approach. For this purpose, a representative cationic metabolite mixture in water, pretreated human plasma, and urine samples spiked with the same metabolite mixture were used and distributed for analysis by all laboratories. The μ eff was determined for all metabolites spiked into each sample. The background electrolyte (BGE) was prepared and employed by each participating lab following the same protocol. All other parameters (capillary, interface, injection volume, voltage ramp, temperature, capillary conditioning, and rinsing procedure, etc.) were left to the discretion of the contributing laboratories. The results revealed that the reproducibility of the μ eff for 20 out of the 21 model compounds was below 3.1% vs 10.9% for RMT, regardless of the huge heterogeneity in experimental conditions and platforms across the 13 laboratories. Overall, this Metabo-ring trial demonstrated that CE-MS is a viable and reproducible approach for metabolomics.

Original language	English
Pages (from-to)	14103-14112
Number of pages	10
Journal	Analytical Chemistry
Volume	92
Issue number	20
DOIs	https://doi.org/10.1021/acs.analchem.0c03129
Publication status	E-pub ahead of print - 22 Sept 2020

ASJC Scopus subject areas

Analytical Chemistry

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Drouin, N., Van Mever, M., Tobolkina, E., Ferre, S., Servais, A-C., Gou, M-J., Nyssen, L., Fillet, M., Lageveen-Kammeijer, G. S. M., Nouta, J., Chetwynd, A. J., Lynch, I., Thorn, J. A., Meixner, J., Loessner, C., Taverna, M., Liu, S., Tran, N. T., Francois, Y. N., ... Ramautar, R. (2020). Capillary electrophoresis-Mass spectrometry at Trial by Metabo-ring: Effective electrophoretic mobility for Reproducible and Robust Compound Annotation. Analytical Chemistry, 92(20), 14103-14112. Advance online publication. https://doi.org/10.1021/acs.analchem.0c03129

@article{3154177fbaa74f1ba8fa9d46cd061774,

title = "Capillary electrophoresis-Mass spectrometry at Trial by Metabo-ring: Effective electrophoretic mobility for Reproducible and Robust Compound Annotation",

abstract = "Capillary zone electrophoresis-mass spectrometry (CE-MS) is a mature analytical tool for the efficient profiling of (highly) polar and ionizable compounds. However, the use of CE-MS in comparison to other separation techniques remains underrepresented in metabolomics, as this analytical approach is still perceived as technically challenging and less reproducible, notably for migration time. The latter is key for a reliable comparison of metabolic profiles and for unknown biomarker identification that is complementary to high resolution MS/MS. In this work, we present the results of a Metabo-ring trial involving 16 CE-MS platforms among 13 different laboratories spanning two continents. The goal was to assess the reproducibility and identification capability of CE-MS by employing effective electrophoretic mobility (μ eff) as the key parameter in comparison to the relative migration time (RMT) approach. For this purpose, a representative cationic metabolite mixture in water, pretreated human plasma, and urine samples spiked with the same metabolite mixture were used and distributed for analysis by all laboratories. The μ eff was determined for all metabolites spiked into each sample. The background electrolyte (BGE) was prepared and employed by each participating lab following the same protocol. All other parameters (capillary, interface, injection volume, voltage ramp, temperature, capillary conditioning, and rinsing procedure, etc.) were left to the discretion of the contributing laboratories. The results revealed that the reproducibility of the μ eff for 20 out of the 21 model compounds was below 3.1% vs 10.9% for RMT, regardless of the huge heterogeneity in experimental conditions and platforms across the 13 laboratories. Overall, this Metabo-ring trial demonstrated that CE-MS is a viable and reproducible approach for metabolomics. ",

author = "Nicolas Drouin and {Van Mever}, Marlien and Elena Tobolkina and Sabrina Ferre and Anne-Catherine Servais and Marie-Jia Gou and Laurent Nyssen and Marianne Fillet and Lageveen-Kammeijer, {Guinevere S M} and Jan Nouta and Chetwynd, {Andrew J} and Iseult Lynch and Thorn, {James A} and Jens Meixner and Christopher Loessner and Myriam Taverna and Sylvie Liu and Tran, {N Thuy} and Francois, {Yannis Nicolas} and Antony Lechner and Reine Nehm{\'e} and {Al Hamoui Dit Banni}, Ghassan and Rouba Nasreddine and Cyril Colas and Lindner, {Herbert H} and Klaus Faserl and Christian Neus{\"u}{\ss} and Manuel Nelke and Stefan Laemmerer and Catherine Perrin and Claudia Bich and Coral Barbas and {\'A}ngeles L{\'o}pez-Gonz{\'a}lvez and Andras Guttman and Marton Szigeti and Philip Britz-McKibbin and Zachary Kroezen and Meera Shanmuganathan and Peter Nemes and Portero, {Erika P} and Thomas Hankemeier and Santiago Codesido and V{\'i}ctor Gonz{\'a}lez-Ruiz and Serge Rudaz and Rawi Ramautar",

year = "2020",

month = sep,

day = "22",

doi = "10.1021/acs.analchem.0c03129",

language = "English",

volume = "92",

pages = "14103--14112",

journal = "Analytical Chemistry",

issn = "0003-2700",

publisher = "American Chemical Society",

number = "20",

}

Drouin, N, Van Mever, M, Tobolkina, E, Ferre, S, Servais, A-C, Gou, M-J, Nyssen, L, Fillet, M, Lageveen-Kammeijer, GSM, Nouta, J, Chetwynd, AJ, Lynch, I, Thorn, JA, Meixner, J, Loessner, C, Taverna, M, Liu, S, Tran, NT, Francois, YN, Lechner, A, Nehmé, R, Al Hamoui Dit Banni, G, Nasreddine, R, Colas, C, Lindner, HH, Faserl, K, Neusüß, C, Nelke, M, Laemmerer, S, Perrin, C, Bich, C, Barbas, C, López-Gonzálvez, Á, Guttman, A, Szigeti, M, Britz-McKibbin, P, Kroezen, Z, Shanmuganathan, M, Nemes, P, Portero, EP, Hankemeier, T, Codesido, S, González-Ruiz, V, Rudaz, S & Ramautar, R 2020, 'Capillary electrophoresis-Mass spectrometry at Trial by Metabo-ring: Effective electrophoretic mobility for Reproducible and Robust Compound Annotation', Analytical Chemistry, vol. 92, no. 20, pp. 14103-14112. https://doi.org/10.1021/acs.analchem.0c03129

TY - JOUR

T1 - Capillary electrophoresis-Mass spectrometry at Trial by Metabo-ring

T2 - Effective electrophoretic mobility for Reproducible and Robust Compound Annotation

AU - Drouin, Nicolas

AU - Van Mever, Marlien

AU - Tobolkina, Elena

AU - Ferre, Sabrina

AU - Servais, Anne-Catherine

AU - Gou, Marie-Jia

AU - Nyssen, Laurent

AU - Fillet, Marianne

AU - Lageveen-Kammeijer, Guinevere S M

AU - Nouta, Jan

AU - Chetwynd, Andrew J

AU - Lynch, Iseult

AU - Thorn, James A

AU - Meixner, Jens

AU - Loessner, Christopher

AU - Taverna, Myriam

AU - Liu, Sylvie

AU - Tran, N Thuy

AU - Francois, Yannis Nicolas

AU - Lechner, Antony

AU - Nehmé, Reine

AU - Al Hamoui Dit Banni, Ghassan

AU - Nasreddine, Rouba

AU - Colas, Cyril

AU - Lindner, Herbert H

AU - Faserl, Klaus

AU - Neusüß, Christian

AU - Nelke, Manuel

AU - Laemmerer, Stefan

AU - Perrin, Catherine

AU - Bich, Claudia

AU - Barbas, Coral

AU - López-Gonzálvez, Ángeles

AU - Guttman, Andras

AU - Szigeti, Marton

AU - Britz-McKibbin, Philip

AU - Kroezen, Zachary

AU - Shanmuganathan, Meera

AU - Nemes, Peter

AU - Portero, Erika P

AU - Hankemeier, Thomas

AU - Codesido, Santiago

AU - González-Ruiz, Víctor

AU - Rudaz, Serge

AU - Ramautar, Rawi

PY - 2020/9/22

Y1 - 2020/9/22

N2 - Capillary zone electrophoresis-mass spectrometry (CE-MS) is a mature analytical tool for the efficient profiling of (highly) polar and ionizable compounds. However, the use of CE-MS in comparison to other separation techniques remains underrepresented in metabolomics, as this analytical approach is still perceived as technically challenging and less reproducible, notably for migration time. The latter is key for a reliable comparison of metabolic profiles and for unknown biomarker identification that is complementary to high resolution MS/MS. In this work, we present the results of a Metabo-ring trial involving 16 CE-MS platforms among 13 different laboratories spanning two continents. The goal was to assess the reproducibility and identification capability of CE-MS by employing effective electrophoretic mobility (μ eff) as the key parameter in comparison to the relative migration time (RMT) approach. For this purpose, a representative cationic metabolite mixture in water, pretreated human plasma, and urine samples spiked with the same metabolite mixture were used and distributed for analysis by all laboratories. The μ eff was determined for all metabolites spiked into each sample. The background electrolyte (BGE) was prepared and employed by each participating lab following the same protocol. All other parameters (capillary, interface, injection volume, voltage ramp, temperature, capillary conditioning, and rinsing procedure, etc.) were left to the discretion of the contributing laboratories. The results revealed that the reproducibility of the μ eff for 20 out of the 21 model compounds was below 3.1% vs 10.9% for RMT, regardless of the huge heterogeneity in experimental conditions and platforms across the 13 laboratories. Overall, this Metabo-ring trial demonstrated that CE-MS is a viable and reproducible approach for metabolomics.

AB - Capillary zone electrophoresis-mass spectrometry (CE-MS) is a mature analytical tool for the efficient profiling of (highly) polar and ionizable compounds. However, the use of CE-MS in comparison to other separation techniques remains underrepresented in metabolomics, as this analytical approach is still perceived as technically challenging and less reproducible, notably for migration time. The latter is key for a reliable comparison of metabolic profiles and for unknown biomarker identification that is complementary to high resolution MS/MS. In this work, we present the results of a Metabo-ring trial involving 16 CE-MS platforms among 13 different laboratories spanning two continents. The goal was to assess the reproducibility and identification capability of CE-MS by employing effective electrophoretic mobility (μ eff) as the key parameter in comparison to the relative migration time (RMT) approach. For this purpose, a representative cationic metabolite mixture in water, pretreated human plasma, and urine samples spiked with the same metabolite mixture were used and distributed for analysis by all laboratories. The μ eff was determined for all metabolites spiked into each sample. The background electrolyte (BGE) was prepared and employed by each participating lab following the same protocol. All other parameters (capillary, interface, injection volume, voltage ramp, temperature, capillary conditioning, and rinsing procedure, etc.) were left to the discretion of the contributing laboratories. The results revealed that the reproducibility of the μ eff for 20 out of the 21 model compounds was below 3.1% vs 10.9% for RMT, regardless of the huge heterogeneity in experimental conditions and platforms across the 13 laboratories. Overall, this Metabo-ring trial demonstrated that CE-MS is a viable and reproducible approach for metabolomics.

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U2 - 10.1021/acs.analchem.0c03129

DO - 10.1021/acs.analchem.0c03129

M3 - Article

C2 - 32961048

SN - 0003-2700

VL - 92

SP - 14103

EP - 14112

JO - Analytical Chemistry

JF - Analytical Chemistry

IS - 20

ER -

Capillary electrophoresis-Mass spectrometry at Trial by Metabo-ring: Effective electrophoretic mobility for Reproducible and Robust Compound Annotation

Abstract

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