Multiplexed micronutrient, inflammation, and malarial antigenemia assessment using a plasma fractionation device

Processing and storing blood samples for future analysis of biomarkers can be challenging in resource limited environments. The preparation of dried blood spots (DBS) from finger-stick collection of whole blood is a widely used and established method as DBS are biosafe, and allow simpler field proce...

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Autores principales: Brindle, Eleanor, Lillis, Lorraine, Barney, Rebecca, Bansil, Pooja, Arredondo, Francisco, Craft, Neal E., Murphy, Eileen, Boyle, David S.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2022
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9678258/
https://www.ncbi.nlm.nih.gov/pubmed/36409692
http://dx.doi.org/10.1371/journal.pone.0277835
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author Brindle, Eleanor
Lillis, Lorraine
Barney, Rebecca
Bansil, Pooja
Arredondo, Francisco
Craft, Neal E.
Murphy, Eileen
Boyle, David S.
author_facet Brindle, Eleanor
Lillis, Lorraine
Barney, Rebecca
Bansil, Pooja
Arredondo, Francisco
Craft, Neal E.
Murphy, Eileen
Boyle, David S.
author_sort Brindle, Eleanor
collection PubMed
description Processing and storing blood samples for future analysis of biomarkers can be challenging in resource limited environments. The preparation of dried blood spots (DBS) from finger-stick collection of whole blood is a widely used and established method as DBS are biosafe, and allow simpler field processing, storage, and transport protocols than serum or plasma. Therefore, DBS are commonly used in population surveys to assess infectious disease and/or micronutrient status. Recently, we reported that DBS can be used with the Q-plex(™) Human Micronutrient 7-plex Array (MN 7-plex), a multiplexed immunoassay. This tool can simultaneously quantify seven protein biomarkers related to micronutrient deficiencies (iodine, iron and vitamin A), inflammation, and malarial antigenemia using plasma or serum. Serum ferritin, an iron biomarker, cannot be measured from DBS due to red blood cell (RBC) ferritin content confounding the results. In this study, we assess a simple blood fractionation tool that passively separates plasma from other blood components via diffusion through a membrane into a plasma collection disc (PCD). We evaluated the concordance of MN 7-plex analyte concentrations from matched panels of eighty-eight samples of PCD, DBS, and wet plasma prepared from anticoagulated venous whole blood. The results showed good correlations of >0.93 between the eluates from PCD and DBS for each analyte except ferritin; while correlations seen for plasma/PCD were weaker. However, the recovery rate of the analytes from the PCD were better than those from DBS. The serum ferritin measures from the PCD were highly correlated to wet plasma samples (0.85). This suggests that surveillance for iron status in low resource settings can be improved over the current methods restricted to only measuring sTfR in DBS. When used in combination with the MN 7-plex, all seven biomarkers can be simultaneously measured using eluates from the PCDs.
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spelling pubmed-96782582022-11-22 Multiplexed micronutrient, inflammation, and malarial antigenemia assessment using a plasma fractionation device Brindle, Eleanor Lillis, Lorraine Barney, Rebecca Bansil, Pooja Arredondo, Francisco Craft, Neal E. Murphy, Eileen Boyle, David S. PLoS One Research Article Processing and storing blood samples for future analysis of biomarkers can be challenging in resource limited environments. The preparation of dried blood spots (DBS) from finger-stick collection of whole blood is a widely used and established method as DBS are biosafe, and allow simpler field processing, storage, and transport protocols than serum or plasma. Therefore, DBS are commonly used in population surveys to assess infectious disease and/or micronutrient status. Recently, we reported that DBS can be used with the Q-plex(™) Human Micronutrient 7-plex Array (MN 7-plex), a multiplexed immunoassay. This tool can simultaneously quantify seven protein biomarkers related to micronutrient deficiencies (iodine, iron and vitamin A), inflammation, and malarial antigenemia using plasma or serum. Serum ferritin, an iron biomarker, cannot be measured from DBS due to red blood cell (RBC) ferritin content confounding the results. In this study, we assess a simple blood fractionation tool that passively separates plasma from other blood components via diffusion through a membrane into a plasma collection disc (PCD). We evaluated the concordance of MN 7-plex analyte concentrations from matched panels of eighty-eight samples of PCD, DBS, and wet plasma prepared from anticoagulated venous whole blood. The results showed good correlations of >0.93 between the eluates from PCD and DBS for each analyte except ferritin; while correlations seen for plasma/PCD were weaker. However, the recovery rate of the analytes from the PCD were better than those from DBS. The serum ferritin measures from the PCD were highly correlated to wet plasma samples (0.85). This suggests that surveillance for iron status in low resource settings can be improved over the current methods restricted to only measuring sTfR in DBS. When used in combination with the MN 7-plex, all seven biomarkers can be simultaneously measured using eluates from the PCDs. Public Library of Science 2022-11-21 /pmc/articles/PMC9678258/ /pubmed/36409692 http://dx.doi.org/10.1371/journal.pone.0277835 Text en © 2022 Brindle et al https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Brindle, Eleanor
Lillis, Lorraine
Barney, Rebecca
Bansil, Pooja
Arredondo, Francisco
Craft, Neal E.
Murphy, Eileen
Boyle, David S.
Multiplexed micronutrient, inflammation, and malarial antigenemia assessment using a plasma fractionation device
title Multiplexed micronutrient, inflammation, and malarial antigenemia assessment using a plasma fractionation device
title_full Multiplexed micronutrient, inflammation, and malarial antigenemia assessment using a plasma fractionation device
title_fullStr Multiplexed micronutrient, inflammation, and malarial antigenemia assessment using a plasma fractionation device
title_full_unstemmed Multiplexed micronutrient, inflammation, and malarial antigenemia assessment using a plasma fractionation device
title_short Multiplexed micronutrient, inflammation, and malarial antigenemia assessment using a plasma fractionation device
title_sort multiplexed micronutrient, inflammation, and malarial antigenemia assessment using a plasma fractionation device
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9678258/
https://www.ncbi.nlm.nih.gov/pubmed/36409692
http://dx.doi.org/10.1371/journal.pone.0277835
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