Analysis of 1508 Plasma Samples by Capillary-Flow Data-Independent Acquisition Profiles Proteomics of Weight Loss and Maintenance

Comprehensive, high throughput analysis of the plasma proteome has the potential to enable holistic analysis of the health state of an individual. Based on our own experience and the evaluation of recent large-scale plasma mass spectrometry (MS) based proteomic studies, we identified two outstanding...

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Autores principales: Bruderer, Roland, Muntel, Jan, Müller, Sebastian, Bernhardt, Oliver M., Gandhi, Tejas, Cominetti, Ornella, Macron, Charlotte, Carayol, Jérôme, Rinner, Oliver, Astrup, Arne, Saris, Wim H.M., Hager, Jörg, Valsesia, Armand, Dayon, Loïc, Reiter, Lukas
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The American Society for Biochemistry and Molecular Biology 2019
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6553938/
https://www.ncbi.nlm.nih.gov/pubmed/30948622
http://dx.doi.org/10.1074/mcp.RA118.001288
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author Bruderer, Roland
Muntel, Jan
Müller, Sebastian
Bernhardt, Oliver M.
Gandhi, Tejas
Cominetti, Ornella
Macron, Charlotte
Carayol, Jérôme
Rinner, Oliver
Astrup, Arne
Saris, Wim H.M.
Hager, Jörg
Valsesia, Armand
Dayon, Loïc
Reiter, Lukas
author_facet Bruderer, Roland
Muntel, Jan
Müller, Sebastian
Bernhardt, Oliver M.
Gandhi, Tejas
Cominetti, Ornella
Macron, Charlotte
Carayol, Jérôme
Rinner, Oliver
Astrup, Arne
Saris, Wim H.M.
Hager, Jörg
Valsesia, Armand
Dayon, Loïc
Reiter, Lukas
author_sort Bruderer, Roland
collection PubMed
description Comprehensive, high throughput analysis of the plasma proteome has the potential to enable holistic analysis of the health state of an individual. Based on our own experience and the evaluation of recent large-scale plasma mass spectrometry (MS) based proteomic studies, we identified two outstanding challenges: slow and delicate nano-flow liquid chromatography (LC) and irreproducibility of identification of data-dependent acquisition (DDA). We determined an optimal solution reducing these limitations with robust capillary-flow data-independent acquisition (DIA) MS. This platform can measure 31 plasma proteomes per day. Using this setup, we acquired a large-scale plasma study of the diet, obesity and genes dietary (DiOGenes) comprising 1508 samples. Proving the robustness, the complete acquisition was achieved on a single analytical column. Totally, 565 proteins (459 identified with two or more peptide sequences) were profiled with 74% data set completeness. On average 408 proteins (5246 peptides) were identified per acquisition (319 proteins in 90% of all acquisitions). The workflow reproducibility was assessed using 34 quality control pools acquired at regular intervals, resulting in 92% data set completeness with CVs for protein measurements of 10.9%. The profiles of 20 apolipoproteins could be profiled revealing distinct changes. The weight loss and weight maintenance resulted in sustained effects on low-grade inflammation, as well as steroid hormone and lipid metabolism, indicating beneficial effects. Comparison to other large-scale plasma weight loss studies demonstrated high robustness and quality of biomarker candidates identified. Tracking of nonenzymatic glycation indicated a delayed, slight reduction of glycation in the weight maintenance phase. Using stable-isotope-references, we could directly and absolutely quantify 60 proteins in the DIA. In conclusion, we present herein the first large-scale plasma DIA study and one of the largest clinical research proteomic studies to date. Application of this fast and robust workflow has great potential to advance biomarker discovery in plasma.
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spelling pubmed-65539382019-06-17 Analysis of 1508 Plasma Samples by Capillary-Flow Data-Independent Acquisition Profiles Proteomics of Weight Loss and Maintenance Bruderer, Roland Muntel, Jan Müller, Sebastian Bernhardt, Oliver M. Gandhi, Tejas Cominetti, Ornella Macron, Charlotte Carayol, Jérôme Rinner, Oliver Astrup, Arne Saris, Wim H.M. Hager, Jörg Valsesia, Armand Dayon, Loïc Reiter, Lukas Mol Cell Proteomics Research Comprehensive, high throughput analysis of the plasma proteome has the potential to enable holistic analysis of the health state of an individual. Based on our own experience and the evaluation of recent large-scale plasma mass spectrometry (MS) based proteomic studies, we identified two outstanding challenges: slow and delicate nano-flow liquid chromatography (LC) and irreproducibility of identification of data-dependent acquisition (DDA). We determined an optimal solution reducing these limitations with robust capillary-flow data-independent acquisition (DIA) MS. This platform can measure 31 plasma proteomes per day. Using this setup, we acquired a large-scale plasma study of the diet, obesity and genes dietary (DiOGenes) comprising 1508 samples. Proving the robustness, the complete acquisition was achieved on a single analytical column. Totally, 565 proteins (459 identified with two or more peptide sequences) were profiled with 74% data set completeness. On average 408 proteins (5246 peptides) were identified per acquisition (319 proteins in 90% of all acquisitions). The workflow reproducibility was assessed using 34 quality control pools acquired at regular intervals, resulting in 92% data set completeness with CVs for protein measurements of 10.9%. The profiles of 20 apolipoproteins could be profiled revealing distinct changes. The weight loss and weight maintenance resulted in sustained effects on low-grade inflammation, as well as steroid hormone and lipid metabolism, indicating beneficial effects. Comparison to other large-scale plasma weight loss studies demonstrated high robustness and quality of biomarker candidates identified. Tracking of nonenzymatic glycation indicated a delayed, slight reduction of glycation in the weight maintenance phase. Using stable-isotope-references, we could directly and absolutely quantify 60 proteins in the DIA. In conclusion, we present herein the first large-scale plasma DIA study and one of the largest clinical research proteomic studies to date. Application of this fast and robust workflow has great potential to advance biomarker discovery in plasma. The American Society for Biochemistry and Molecular Biology 2019-06 2019-04-04 /pmc/articles/PMC6553938/ /pubmed/30948622 http://dx.doi.org/10.1074/mcp.RA118.001288 Text en © 2019 Bruderer et al. Published by The American Society for Biochemistry and Molecular Biology, Inc. Author's Choice—Final version open access under the terms of the Creative Commons CC-BY license (http://creativecommons.org/licenses/by/4.0) .
spellingShingle Research
Bruderer, Roland
Muntel, Jan
Müller, Sebastian
Bernhardt, Oliver M.
Gandhi, Tejas
Cominetti, Ornella
Macron, Charlotte
Carayol, Jérôme
Rinner, Oliver
Astrup, Arne
Saris, Wim H.M.
Hager, Jörg
Valsesia, Armand
Dayon, Loïc
Reiter, Lukas
Analysis of 1508 Plasma Samples by Capillary-Flow Data-Independent Acquisition Profiles Proteomics of Weight Loss and Maintenance
title Analysis of 1508 Plasma Samples by Capillary-Flow Data-Independent Acquisition Profiles Proteomics of Weight Loss and Maintenance
title_full Analysis of 1508 Plasma Samples by Capillary-Flow Data-Independent Acquisition Profiles Proteomics of Weight Loss and Maintenance
title_fullStr Analysis of 1508 Plasma Samples by Capillary-Flow Data-Independent Acquisition Profiles Proteomics of Weight Loss and Maintenance
title_full_unstemmed Analysis of 1508 Plasma Samples by Capillary-Flow Data-Independent Acquisition Profiles Proteomics of Weight Loss and Maintenance
title_short Analysis of 1508 Plasma Samples by Capillary-Flow Data-Independent Acquisition Profiles Proteomics of Weight Loss and Maintenance
title_sort analysis of 1508 plasma samples by capillary-flow data-independent acquisition profiles proteomics of weight loss and maintenance
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6553938/
https://www.ncbi.nlm.nih.gov/pubmed/30948622
http://dx.doi.org/10.1074/mcp.RA118.001288
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