Ex vivo instability of lipids in whole blood: preanalytical recommendations for clinical lipidomics studies

Reliability, robustness, and interlaboratory comparability of quantitative measurements is critical for clinical lipidomics studies. Lipids’ different ex vivo stability in blood bears the risk of misinterpretation of data. Clear recommendations for the process of blood sample collection are required...

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Autores principales: Wang, Qingqing, Hoene, Miriam, Hu, Chunxiu, Fritsche, Louise, Ahrends, Robert, Liebisch, Gerhard, Ekroos, Kim, Fritsche, Andreas, Birkenfeld, Andreas L., Liu, Xinyu, Zhao, Xinjie, Li, Qi, Su, Benzhe, Peter, Andreas, Xu, Guowang, Lehmann, Rainer
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Biochemistry and Molecular Biology 2023
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10208886/
https://www.ncbi.nlm.nih.gov/pubmed/37087100
http://dx.doi.org/10.1016/j.jlr.2023.100378
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author Wang, Qingqing
Hoene, Miriam
Hu, Chunxiu
Fritsche, Louise
Ahrends, Robert
Liebisch, Gerhard
Ekroos, Kim
Fritsche, Andreas
Birkenfeld, Andreas L.
Liu, Xinyu
Zhao, Xinjie
Li, Qi
Su, Benzhe
Peter, Andreas
Xu, Guowang
Lehmann, Rainer
author_facet Wang, Qingqing
Hoene, Miriam
Hu, Chunxiu
Fritsche, Louise
Ahrends, Robert
Liebisch, Gerhard
Ekroos, Kim
Fritsche, Andreas
Birkenfeld, Andreas L.
Liu, Xinyu
Zhao, Xinjie
Li, Qi
Su, Benzhe
Peter, Andreas
Xu, Guowang
Lehmann, Rainer
author_sort Wang, Qingqing
collection PubMed
description Reliability, robustness, and interlaboratory comparability of quantitative measurements is critical for clinical lipidomics studies. Lipids’ different ex vivo stability in blood bears the risk of misinterpretation of data. Clear recommendations for the process of blood sample collection are required. We studied by UHPLC-high resolution mass spectrometry, as part of the “Preanalytics interest group” of the International Lipidomics Society, the stability of 417 lipid species in EDTA whole blood after exposure to either 4°C, 21°C, or 30°C at six different time points (0.5 h–24 h) to cover common daily routine conditions in clinical settings. In total, >800 samples were analyzed. 325 and 288 robust lipid species resisted 24 h exposure of EDTA whole blood to 21°C or 30°C, respectively. Most significant instabilities were detected for FA, LPE, and LPC. Based on our data, we recommend cooling whole blood at once and permanent. Plasma should be separated within 4 h, unless the focus is solely on robust lipids. Lists are provided to check the ex vivo (in)stability of distinct lipids and potential biomarkers of interest in whole blood. To conclude, our results contribute to the international efforts towards reliable and comparable clinical lipidomics data paving the way to the proper diagnostic application of distinct lipid patterns or lipid profiles in the future.
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spelling pubmed-102088862023-05-26 Ex vivo instability of lipids in whole blood: preanalytical recommendations for clinical lipidomics studies Wang, Qingqing Hoene, Miriam Hu, Chunxiu Fritsche, Louise Ahrends, Robert Liebisch, Gerhard Ekroos, Kim Fritsche, Andreas Birkenfeld, Andreas L. Liu, Xinyu Zhao, Xinjie Li, Qi Su, Benzhe Peter, Andreas Xu, Guowang Lehmann, Rainer J Lipid Res Research Article Reliability, robustness, and interlaboratory comparability of quantitative measurements is critical for clinical lipidomics studies. Lipids’ different ex vivo stability in blood bears the risk of misinterpretation of data. Clear recommendations for the process of blood sample collection are required. We studied by UHPLC-high resolution mass spectrometry, as part of the “Preanalytics interest group” of the International Lipidomics Society, the stability of 417 lipid species in EDTA whole blood after exposure to either 4°C, 21°C, or 30°C at six different time points (0.5 h–24 h) to cover common daily routine conditions in clinical settings. In total, >800 samples were analyzed. 325 and 288 robust lipid species resisted 24 h exposure of EDTA whole blood to 21°C or 30°C, respectively. Most significant instabilities were detected for FA, LPE, and LPC. Based on our data, we recommend cooling whole blood at once and permanent. Plasma should be separated within 4 h, unless the focus is solely on robust lipids. Lists are provided to check the ex vivo (in)stability of distinct lipids and potential biomarkers of interest in whole blood. To conclude, our results contribute to the international efforts towards reliable and comparable clinical lipidomics data paving the way to the proper diagnostic application of distinct lipid patterns or lipid profiles in the future. American Society for Biochemistry and Molecular Biology 2023-04-21 /pmc/articles/PMC10208886/ /pubmed/37087100 http://dx.doi.org/10.1016/j.jlr.2023.100378 Text en © 2023 The Authors https://creativecommons.org/licenses/by/4.0/This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Research Article
Wang, Qingqing
Hoene, Miriam
Hu, Chunxiu
Fritsche, Louise
Ahrends, Robert
Liebisch, Gerhard
Ekroos, Kim
Fritsche, Andreas
Birkenfeld, Andreas L.
Liu, Xinyu
Zhao, Xinjie
Li, Qi
Su, Benzhe
Peter, Andreas
Xu, Guowang
Lehmann, Rainer
Ex vivo instability of lipids in whole blood: preanalytical recommendations for clinical lipidomics studies
title Ex vivo instability of lipids in whole blood: preanalytical recommendations for clinical lipidomics studies
title_full Ex vivo instability of lipids in whole blood: preanalytical recommendations for clinical lipidomics studies
title_fullStr Ex vivo instability of lipids in whole blood: preanalytical recommendations for clinical lipidomics studies
title_full_unstemmed Ex vivo instability of lipids in whole blood: preanalytical recommendations for clinical lipidomics studies
title_short Ex vivo instability of lipids in whole blood: preanalytical recommendations for clinical lipidomics studies
title_sort ex vivo instability of lipids in whole blood: preanalytical recommendations for clinical lipidomics studies
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10208886/
https://www.ncbi.nlm.nih.gov/pubmed/37087100
http://dx.doi.org/10.1016/j.jlr.2023.100378
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