International ring trial of a high resolution targeted metabolomics and lipidomics platform for serum and plasma analysis

J. Will Thompson; Kendra J. Adams; Jerzy Adamski; Yasmin Asad; David Borts; John A. Bowden; Gregory Byram; Viet Dang; Warwick Dunn; Facundo Fernandez; Oliver Fiehn; David A. Gaul; Andreas FR Hühmer; Anastasia Kalli; Therese  Koal; Stormy Koeniger; Rupasri Mandal; Florian Meier; Naser Fuad J.; Donna O'Neil; Akos Pal; Gary J. Patti; Hai  Pham-Tuan; Cornelia Prehn; Florence I. Raynaud; Tong Shen; Andrew Southam; Lisa St. John-Williams; Karolina Sulek; Catherine G. Vasilopoulou; Mark Viant; Cate Winder; David Wishart; Lun Zhang; Jiamin Zheng; M. Arthur Moseley

doi:10.1021/acs.analchem.9b02908

International ring trial of a high resolution targeted metabolomics and lipidomics platform for serum and plasma analysis

J. Will Thompson, Kendra J. Adams, Jerzy Adamski, Yasmin Asad, David Borts, John A. Bowden, Gregory Byram, Viet Dang, Warwick Dunn, Facundo Fernandez, Oliver Fiehn, David A. Gaul, Andreas FR Hühmer, Anastasia Kalli, Therese Koal, Stormy Koeniger, Rupasri Mandal, Florian Meier, Naser Fuad J., Donna O'NeilAkos Pal, Gary J. Patti, Hai Pham-Tuan, Cornelia Prehn, Florence I. Raynaud, Tong Shen, Andrew Southam, Lisa St. John-Williams, Karolina Sulek, Catherine G. Vasilopoulou, Mark Viant, Cate Winder, David Wishart, Lun Zhang, Jiamin Zheng, M. Arthur Moseley

Biosciences

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Abstract

A challenge facing metabolomics in the analysis of large human cohorts is the cross-laboratory comparability of quantitative metabolomics measurements. In this study, 14 laboratories analyzed various blood specimens using a common experimental protocol provided with the Biocrates AbsoluteIDQ p400HR kit, to quantify up to 408 metabolites. The specimens included human plasma and serum from male and female donors, mouse and rat plasma, as well as NIST SRM 1950 reference plasma. The metabolite classes covered range from polar (e.g., amino acids and biogenic amines) to nonpolar (e.g., diacyl-and triacyl-glycerols), and they span 11 common metabolite classes. The manuscript describes a strict system suitability testing (SST) criteria used to evaluate each laboratory's readiness to perform the assay, and provides the SST Skyline documents for public dissemination. The study found approximately 250 metabolites were routinely quantified in the sample types tested, using Orbitrap instruments. Interlaboratory variance for the NIST SRM-1950 has a median of 10% for amino acids, 24% for biogenic amines, 38% for acylcarnitines, 25% for glycerolipids, 23% for glycerophospholipids, 16% for cholesteryl esters, 15% for sphingolipids, and 9% for hexoses. Comparing to consensus values for NIST SRM-1950, nearly 80% of comparable analytes demonstrated bias of <50% from the reference value. The findings of this study result in recommendations of best practices for system suitability, quality control, and calibration. We demonstrate that with appropriate controls, high-resolution metabolomics can provide accurate results with good precision across laboratories, and the p400HR therefore is a reliable approach for generating consistent and comparable metabolomics data.

Original language	English
Article number	9b02908
Pages (from-to)	14407-14416
Number of pages	10
Journal	Analytical Chemistry
Volume	91
Issue number	22
Early online date	22 Oct 2019
DOIs	https://doi.org/10.1021/acs.analchem.9b02908
Publication status	Published - 19 Nov 2019

ASJC Scopus subject areas

Analytical Chemistry

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This document is the Accepted Manuscript version of a Published Work that appeared in final form in Analytical Chemistry, copyright © American Chemical Society after peer review and technical editing by the publisher. To access the final edited and published work see 10.1021/acs.analchem.9b02908
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Thompson, J. W., Adams, K. J., Adamski, J., Asad, Y., Borts, D., Bowden, J. A., Byram, G., Dang, V., Dunn, W., Fernandez, F., Fiehn, O., Gaul, D. A., Hühmer, A. FR., Kalli, A., Koal, T., Koeniger, S., Mandal, R., Meier, F., Fuad J., N., ... Moseley, M. A. (2019). International ring trial of a high resolution targeted metabolomics and lipidomics platform for serum and plasma analysis. Analytical Chemistry, 91(22), 14407-14416. Article 9b02908. https://doi.org/10.1021/acs.analchem.9b02908

@article{63e2eae47cc849be87d987e363c646fa,

title = "International ring trial of a high resolution targeted metabolomics and lipidomics platform for serum and plasma analysis",

abstract = "A challenge facing metabolomics in the analysis of large human cohorts is the cross-laboratory comparability of quantitative metabolomics measurements. In this study, 14 laboratories analyzed various blood specimens using a common experimental protocol provided with the Biocrates AbsoluteIDQ p400HR kit, to quantify up to 408 metabolites. The specimens included human plasma and serum from male and female donors, mouse and rat plasma, as well as NIST SRM 1950 reference plasma. The metabolite classes covered range from polar (e.g., amino acids and biogenic amines) to nonpolar (e.g., diacyl-and triacyl-glycerols), and they span 11 common metabolite classes. The manuscript describes a strict system suitability testing (SST) criteria used to evaluate each laboratory's readiness to perform the assay, and provides the SST Skyline documents for public dissemination. The study found approximately 250 metabolites were routinely quantified in the sample types tested, using Orbitrap instruments. Interlaboratory variance for the NIST SRM-1950 has a median of 10% for amino acids, 24% for biogenic amines, 38% for acylcarnitines, 25% for glycerolipids, 23% for glycerophospholipids, 16% for cholesteryl esters, 15% for sphingolipids, and 9% for hexoses. Comparing to consensus values for NIST SRM-1950, nearly 80% of comparable analytes demonstrated bias of <50% from the reference value. The findings of this study result in recommendations of best practices for system suitability, quality control, and calibration. We demonstrate that with appropriate controls, high-resolution metabolomics can provide accurate results with good precision across laboratories, and the p400HR therefore is a reliable approach for generating consistent and comparable metabolomics data.",

author = "Thompson, {J. Will} and Adams, {Kendra J.} and Jerzy Adamski and Yasmin Asad and David Borts and Bowden, {John A.} and Gregory Byram and Viet Dang and Warwick Dunn and Facundo Fernandez and Oliver Fiehn and Gaul, {David A.} and H{\"u}hmer, {Andreas FR} and Anastasia Kalli and Therese Koal and Stormy Koeniger and Rupasri Mandal and Florian Meier and {Fuad J.}, Naser and Donna O'Neil and Akos Pal and Patti, {Gary J.} and Hai Pham-Tuan and Cornelia Prehn and Raynaud, {Florence I.} and Tong Shen and Andrew Southam and {St. John-Williams}, Lisa and Karolina Sulek and Vasilopoulou, {Catherine G.} and Mark Viant and Cate Winder and David Wishart and Lun Zhang and Jiamin Zheng and Moseley, {M. Arthur}",

year = "2019",

month = nov,

day = "19",

doi = "10.1021/acs.analchem.9b02908",

language = "English",

volume = "91",

pages = "14407--14416",

journal = "Analytical Chemistry",

issn = "0003-2700",

publisher = "American Chemical Society",

number = "22",

}

Thompson, JW, Adams, KJ, Adamski, J, Asad, Y, Borts, D, Bowden, JA, Byram, G, Dang, V, Dunn, W, Fernandez, F, Fiehn, O, Gaul, DA, Hühmer, AFR, Kalli, A, Koal, T, Koeniger, S, Mandal, R, Meier, F, Fuad J., N, O'Neil, D, Pal, A, Patti, GJ, Pham-Tuan, H, Prehn, C, Raynaud, FI, Shen, T, Southam, A, St. John-Williams, L, Sulek, K, Vasilopoulou, CG, Viant, M, Winder, C, Wishart, D, Zhang, L, Zheng, J & Moseley, MA 2019, 'International ring trial of a high resolution targeted metabolomics and lipidomics platform for serum and plasma analysis', Analytical Chemistry, vol. 91, no. 22, 9b02908, pp. 14407-14416. https://doi.org/10.1021/acs.analchem.9b02908

TY - JOUR

T1 - International ring trial of a high resolution targeted metabolomics and lipidomics platform for serum and plasma analysis

AU - Thompson, J. Will

AU - Adams, Kendra J.

AU - Adamski, Jerzy

AU - Asad, Yasmin

AU - Borts, David

AU - Bowden, John A.

AU - Byram, Gregory

AU - Dang, Viet

AU - Dunn, Warwick

AU - Fernandez, Facundo

AU - Fiehn, Oliver

AU - Gaul, David A.

AU - Hühmer, Andreas FR

AU - Kalli, Anastasia

AU - Koal, Therese

AU - Koeniger, Stormy

AU - Mandal, Rupasri

AU - Meier, Florian

AU - Fuad J., Naser

AU - O'Neil, Donna

AU - Pal, Akos

AU - Patti, Gary J.

AU - Pham-Tuan, Hai

AU - Prehn, Cornelia

AU - Raynaud, Florence I.

AU - Shen, Tong

AU - Southam, Andrew

AU - St. John-Williams, Lisa

AU - Sulek, Karolina

AU - Vasilopoulou, Catherine G.

AU - Viant, Mark

AU - Winder, Cate

AU - Wishart, David

AU - Zhang, Lun

AU - Zheng, Jiamin

AU - Moseley, M. Arthur

PY - 2019/11/19

Y1 - 2019/11/19

N2 - A challenge facing metabolomics in the analysis of large human cohorts is the cross-laboratory comparability of quantitative metabolomics measurements. In this study, 14 laboratories analyzed various blood specimens using a common experimental protocol provided with the Biocrates AbsoluteIDQ p400HR kit, to quantify up to 408 metabolites. The specimens included human plasma and serum from male and female donors, mouse and rat plasma, as well as NIST SRM 1950 reference plasma. The metabolite classes covered range from polar (e.g., amino acids and biogenic amines) to nonpolar (e.g., diacyl-and triacyl-glycerols), and they span 11 common metabolite classes. The manuscript describes a strict system suitability testing (SST) criteria used to evaluate each laboratory's readiness to perform the assay, and provides the SST Skyline documents for public dissemination. The study found approximately 250 metabolites were routinely quantified in the sample types tested, using Orbitrap instruments. Interlaboratory variance for the NIST SRM-1950 has a median of 10% for amino acids, 24% for biogenic amines, 38% for acylcarnitines, 25% for glycerolipids, 23% for glycerophospholipids, 16% for cholesteryl esters, 15% for sphingolipids, and 9% for hexoses. Comparing to consensus values for NIST SRM-1950, nearly 80% of comparable analytes demonstrated bias of <50% from the reference value. The findings of this study result in recommendations of best practices for system suitability, quality control, and calibration. We demonstrate that with appropriate controls, high-resolution metabolomics can provide accurate results with good precision across laboratories, and the p400HR therefore is a reliable approach for generating consistent and comparable metabolomics data.

AB - A challenge facing metabolomics in the analysis of large human cohorts is the cross-laboratory comparability of quantitative metabolomics measurements. In this study, 14 laboratories analyzed various blood specimens using a common experimental protocol provided with the Biocrates AbsoluteIDQ p400HR kit, to quantify up to 408 metabolites. The specimens included human plasma and serum from male and female donors, mouse and rat plasma, as well as NIST SRM 1950 reference plasma. The metabolite classes covered range from polar (e.g., amino acids and biogenic amines) to nonpolar (e.g., diacyl-and triacyl-glycerols), and they span 11 common metabolite classes. The manuscript describes a strict system suitability testing (SST) criteria used to evaluate each laboratory's readiness to perform the assay, and provides the SST Skyline documents for public dissemination. The study found approximately 250 metabolites were routinely quantified in the sample types tested, using Orbitrap instruments. Interlaboratory variance for the NIST SRM-1950 has a median of 10% for amino acids, 24% for biogenic amines, 38% for acylcarnitines, 25% for glycerolipids, 23% for glycerophospholipids, 16% for cholesteryl esters, 15% for sphingolipids, and 9% for hexoses. Comparing to consensus values for NIST SRM-1950, nearly 80% of comparable analytes demonstrated bias of <50% from the reference value. The findings of this study result in recommendations of best practices for system suitability, quality control, and calibration. We demonstrate that with appropriate controls, high-resolution metabolomics can provide accurate results with good precision across laboratories, and the p400HR therefore is a reliable approach for generating consistent and comparable metabolomics data.

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U2 - 10.1021/acs.analchem.9b02908

DO - 10.1021/acs.analchem.9b02908

M3 - Article

SN - 0003-2700

VL - 91

SP - 14407

EP - 14416

JO - Analytical Chemistry

JF - Analytical Chemistry

IS - 22

M1 - 9b02908

ER -

International ring trial of a high resolution targeted metabolomics and lipidomics platform for serum and plasma analysis

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