Changes to Serum Sample Tube and Processing Methodology Does Not Cause Inter-Individual Variation in Automated Whole Serum N-Glycan Profiling in Health and Disease

INTRODUCTION: Serum N-glycans have been identified as putative biomarkers for numerous diseases. The impact of different serum sample tubes and processing methods on N-glycan analysis has received relatively little attention. This study aimed to determine the effect of different sample tubes and pro...

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Autores principales: Ventham, Nicholas T., Gardner, Richard A., Kennedy, Nicholas A., Shubhakar, Archana, Kalla, Rahul, Nimmo, Elaine R., Fernandes, Daryl L., Satsangi, Jack, Spencer, Daniel I. R.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4382121/
https://www.ncbi.nlm.nih.gov/pubmed/25831126
http://dx.doi.org/10.1371/journal.pone.0123028
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author Ventham, Nicholas T.
Gardner, Richard A.
Kennedy, Nicholas A.
Shubhakar, Archana
Kalla, Rahul
Nimmo, Elaine R.
Fernandes, Daryl L.
Satsangi, Jack
Spencer, Daniel I. R.
author_facet Ventham, Nicholas T.
Gardner, Richard A.
Kennedy, Nicholas A.
Shubhakar, Archana
Kalla, Rahul
Nimmo, Elaine R.
Fernandes, Daryl L.
Satsangi, Jack
Spencer, Daniel I. R.
author_sort Ventham, Nicholas T.
collection PubMed
description INTRODUCTION: Serum N-glycans have been identified as putative biomarkers for numerous diseases. The impact of different serum sample tubes and processing methods on N-glycan analysis has received relatively little attention. This study aimed to determine the effect of different sample tubes and processing methods on the whole serum N-glycan profile in both health and disease. A secondary objective was to describe a robot automated N-glycan release, labeling and cleanup process for use in a biomarker discovery system. METHODS: 25 patients with active and quiescent inflammatory bowel disease and controls had three different serum sample tubes taken at the same draw. Two different processing methods were used for three types of tube (with and without gel-separation medium). Samples were randomised and processed in a blinded fashion. Whole serum N-glycan release, 2-aminobenzamide labeling and cleanup was automated using a Hamilton Microlab STARlet Liquid Handling robot. Samples were analysed using a hydrophilic interaction liquid chromatography/ethylene bridged hybrid(BEH) column on an ultra-high performance liquid chromatography instrument. Data were analysed quantitatively by pairwise correlation and hierarchical clustering using the area under each chromatogram peak. Qualitatively, a blinded assessor attempted to match chromatograms to each individual. RESULTS: There was small intra-individual variation in serum N-glycan profiles from samples collected using different sample processing methods. Intra-individual correlation coefficients were between 0.99 and 1. Unsupervised hierarchical clustering and principal coordinate analyses accurately matched samples from the same individual. Qualitative analysis demonstrated good chromatogram overlay and a blinded assessor was able to accurately match individuals based on chromatogram profile, regardless of disease status. CONCLUSIONS: The three different serum sample tubes processed using the described methods cause minimal inter-individual variation in serum whole N-glycan profile when processed using an automated workstream. This has important implications for N-glycan biomarker discovery studies using different serum processing standard operating procedures.
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spelling pubmed-43821212015-04-09 Changes to Serum Sample Tube and Processing Methodology Does Not Cause Inter-Individual Variation in Automated Whole Serum N-Glycan Profiling in Health and Disease Ventham, Nicholas T. Gardner, Richard A. Kennedy, Nicholas A. Shubhakar, Archana Kalla, Rahul Nimmo, Elaine R. Fernandes, Daryl L. Satsangi, Jack Spencer, Daniel I. R. PLoS One Research Article INTRODUCTION: Serum N-glycans have been identified as putative biomarkers for numerous diseases. The impact of different serum sample tubes and processing methods on N-glycan analysis has received relatively little attention. This study aimed to determine the effect of different sample tubes and processing methods on the whole serum N-glycan profile in both health and disease. A secondary objective was to describe a robot automated N-glycan release, labeling and cleanup process for use in a biomarker discovery system. METHODS: 25 patients with active and quiescent inflammatory bowel disease and controls had three different serum sample tubes taken at the same draw. Two different processing methods were used for three types of tube (with and without gel-separation medium). Samples were randomised and processed in a blinded fashion. Whole serum N-glycan release, 2-aminobenzamide labeling and cleanup was automated using a Hamilton Microlab STARlet Liquid Handling robot. Samples were analysed using a hydrophilic interaction liquid chromatography/ethylene bridged hybrid(BEH) column on an ultra-high performance liquid chromatography instrument. Data were analysed quantitatively by pairwise correlation and hierarchical clustering using the area under each chromatogram peak. Qualitatively, a blinded assessor attempted to match chromatograms to each individual. RESULTS: There was small intra-individual variation in serum N-glycan profiles from samples collected using different sample processing methods. Intra-individual correlation coefficients were between 0.99 and 1. Unsupervised hierarchical clustering and principal coordinate analyses accurately matched samples from the same individual. Qualitative analysis demonstrated good chromatogram overlay and a blinded assessor was able to accurately match individuals based on chromatogram profile, regardless of disease status. CONCLUSIONS: The three different serum sample tubes processed using the described methods cause minimal inter-individual variation in serum whole N-glycan profile when processed using an automated workstream. This has important implications for N-glycan biomarker discovery studies using different serum processing standard operating procedures. Public Library of Science 2015-04-01 /pmc/articles/PMC4382121/ /pubmed/25831126 http://dx.doi.org/10.1371/journal.pone.0123028 Text en © 2015 Ventham et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Ventham, Nicholas T.
Gardner, Richard A.
Kennedy, Nicholas A.
Shubhakar, Archana
Kalla, Rahul
Nimmo, Elaine R.
Fernandes, Daryl L.
Satsangi, Jack
Spencer, Daniel I. R.
Changes to Serum Sample Tube and Processing Methodology Does Not Cause Inter-Individual Variation in Automated Whole Serum N-Glycan Profiling in Health and Disease
title Changes to Serum Sample Tube and Processing Methodology Does Not Cause Inter-Individual Variation in Automated Whole Serum N-Glycan Profiling in Health and Disease
title_full Changes to Serum Sample Tube and Processing Methodology Does Not Cause Inter-Individual Variation in Automated Whole Serum N-Glycan Profiling in Health and Disease
title_fullStr Changes to Serum Sample Tube and Processing Methodology Does Not Cause Inter-Individual Variation in Automated Whole Serum N-Glycan Profiling in Health and Disease
title_full_unstemmed Changes to Serum Sample Tube and Processing Methodology Does Not Cause Inter-Individual Variation in Automated Whole Serum N-Glycan Profiling in Health and Disease
title_short Changes to Serum Sample Tube and Processing Methodology Does Not Cause Inter-Individual Variation in Automated Whole Serum N-Glycan Profiling in Health and Disease
title_sort changes to serum sample tube and processing methodology does not cause inter-individual variation in automated whole serum n-glycan profiling in health and disease
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4382121/
https://www.ncbi.nlm.nih.gov/pubmed/25831126
http://dx.doi.org/10.1371/journal.pone.0123028
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