Parallel Workflow for High-Throughput (>1,000 Samples/Day) Quantitative Analysis of Human Insulin-Like Growth Factor 1 Using Mass Spectrometric Immunoassay

Insulin-like growth factor 1 (IGF1) is an important biomarker for the management of growth hormone disorders. Recently there has been rising interest in deploying mass spectrometric (MS) methods of detection for measuring IGF1. However, widespread clinical adoption of any MS-based IGF1 assay will re...

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Autores principales: Oran, Paul E., Trenchevska, Olgica, Nedelkov, Dobrin, Borges, Chad R., Schaab, Matthew R., Rehder, Douglas S., Jarvis, Jason W., Sherma, Nisha D., Shen, Luhui, Krastins, Bryan, Lopez, Mary F., Schwenke, Dawn C., Reaven, Peter D., Nelson, Randall W.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3963945/
https://www.ncbi.nlm.nih.gov/pubmed/24664114
http://dx.doi.org/10.1371/journal.pone.0092801
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author Oran, Paul E.
Trenchevska, Olgica
Nedelkov, Dobrin
Borges, Chad R.
Schaab, Matthew R.
Rehder, Douglas S.
Jarvis, Jason W.
Sherma, Nisha D.
Shen, Luhui
Krastins, Bryan
Lopez, Mary F.
Schwenke, Dawn C.
Reaven, Peter D.
Nelson, Randall W.
author_facet Oran, Paul E.
Trenchevska, Olgica
Nedelkov, Dobrin
Borges, Chad R.
Schaab, Matthew R.
Rehder, Douglas S.
Jarvis, Jason W.
Sherma, Nisha D.
Shen, Luhui
Krastins, Bryan
Lopez, Mary F.
Schwenke, Dawn C.
Reaven, Peter D.
Nelson, Randall W.
author_sort Oran, Paul E.
collection PubMed
description Insulin-like growth factor 1 (IGF1) is an important biomarker for the management of growth hormone disorders. Recently there has been rising interest in deploying mass spectrometric (MS) methods of detection for measuring IGF1. However, widespread clinical adoption of any MS-based IGF1 assay will require increased throughput and speed to justify the costs of analyses, and robust industrial platforms that are reproducible across laboratories. Presented here is an MS-based quantitative IGF1 assay with performance rating of >1,000 samples/day, and a capability of quantifying IGF1 point mutations and posttranslational modifications. The throughput of the IGF1 mass spectrometric immunoassay (MSIA) benefited from a simplified sample preparation step, IGF1 immunocapture in a tip format, and high-throughput MALDI-TOF MS analysis. The Limit of Detection and Limit of Quantification of the resulting assay were 1.5 μg/L and 5 μg/L, respectively, with intra- and inter-assay precision CVs of less than 10%, and good linearity and recovery characteristics. The IGF1 MSIA was benchmarked against commercially available IGF1 ELISA via Bland-Altman method comparison test, resulting in a slight positive bias of 16%. The IGF1 MSIA was employed in an optimized parallel workflow utilizing two pipetting robots and MALDI-TOF-MS instruments synced into one-hour phases of sample preparation, extraction and MSIA pipette tip elution, MS data collection, and data processing. Using this workflow, high-throughput IGF1 quantification of 1,054 human samples was achieved in approximately 9 hours. This rate of assaying is a significant improvement over existing MS-based IGF1 assays, and is on par with that of the enzyme-based immunoassays. Furthermore, a mutation was detected in ∼1% of the samples (SNP: rs17884626, creating an A→T substitution at position 67 of the IGF1), demonstrating the capability of IGF1 MSIA to detect point mutations and posttranslational modifications.
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spelling pubmed-39639452014-03-27 Parallel Workflow for High-Throughput (>1,000 Samples/Day) Quantitative Analysis of Human Insulin-Like Growth Factor 1 Using Mass Spectrometric Immunoassay Oran, Paul E. Trenchevska, Olgica Nedelkov, Dobrin Borges, Chad R. Schaab, Matthew R. Rehder, Douglas S. Jarvis, Jason W. Sherma, Nisha D. Shen, Luhui Krastins, Bryan Lopez, Mary F. Schwenke, Dawn C. Reaven, Peter D. Nelson, Randall W. PLoS One Research Article Insulin-like growth factor 1 (IGF1) is an important biomarker for the management of growth hormone disorders. Recently there has been rising interest in deploying mass spectrometric (MS) methods of detection for measuring IGF1. However, widespread clinical adoption of any MS-based IGF1 assay will require increased throughput and speed to justify the costs of analyses, and robust industrial platforms that are reproducible across laboratories. Presented here is an MS-based quantitative IGF1 assay with performance rating of >1,000 samples/day, and a capability of quantifying IGF1 point mutations and posttranslational modifications. The throughput of the IGF1 mass spectrometric immunoassay (MSIA) benefited from a simplified sample preparation step, IGF1 immunocapture in a tip format, and high-throughput MALDI-TOF MS analysis. The Limit of Detection and Limit of Quantification of the resulting assay were 1.5 μg/L and 5 μg/L, respectively, with intra- and inter-assay precision CVs of less than 10%, and good linearity and recovery characteristics. The IGF1 MSIA was benchmarked against commercially available IGF1 ELISA via Bland-Altman method comparison test, resulting in a slight positive bias of 16%. The IGF1 MSIA was employed in an optimized parallel workflow utilizing two pipetting robots and MALDI-TOF-MS instruments synced into one-hour phases of sample preparation, extraction and MSIA pipette tip elution, MS data collection, and data processing. Using this workflow, high-throughput IGF1 quantification of 1,054 human samples was achieved in approximately 9 hours. This rate of assaying is a significant improvement over existing MS-based IGF1 assays, and is on par with that of the enzyme-based immunoassays. Furthermore, a mutation was detected in ∼1% of the samples (SNP: rs17884626, creating an A→T substitution at position 67 of the IGF1), demonstrating the capability of IGF1 MSIA to detect point mutations and posttranslational modifications. Public Library of Science 2014-03-24 /pmc/articles/PMC3963945/ /pubmed/24664114 http://dx.doi.org/10.1371/journal.pone.0092801 Text en © 2014 Oran 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
Oran, Paul E.
Trenchevska, Olgica
Nedelkov, Dobrin
Borges, Chad R.
Schaab, Matthew R.
Rehder, Douglas S.
Jarvis, Jason W.
Sherma, Nisha D.
Shen, Luhui
Krastins, Bryan
Lopez, Mary F.
Schwenke, Dawn C.
Reaven, Peter D.
Nelson, Randall W.
Parallel Workflow for High-Throughput (>1,000 Samples/Day) Quantitative Analysis of Human Insulin-Like Growth Factor 1 Using Mass Spectrometric Immunoassay
title Parallel Workflow for High-Throughput (>1,000 Samples/Day) Quantitative Analysis of Human Insulin-Like Growth Factor 1 Using Mass Spectrometric Immunoassay
title_full Parallel Workflow for High-Throughput (>1,000 Samples/Day) Quantitative Analysis of Human Insulin-Like Growth Factor 1 Using Mass Spectrometric Immunoassay
title_fullStr Parallel Workflow for High-Throughput (>1,000 Samples/Day) Quantitative Analysis of Human Insulin-Like Growth Factor 1 Using Mass Spectrometric Immunoassay
title_full_unstemmed Parallel Workflow for High-Throughput (>1,000 Samples/Day) Quantitative Analysis of Human Insulin-Like Growth Factor 1 Using Mass Spectrometric Immunoassay
title_short Parallel Workflow for High-Throughput (>1,000 Samples/Day) Quantitative Analysis of Human Insulin-Like Growth Factor 1 Using Mass Spectrometric Immunoassay
title_sort parallel workflow for high-throughput (>1,000 samples/day) quantitative analysis of human insulin-like growth factor 1 using mass spectrometric immunoassay
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3963945/
https://www.ncbi.nlm.nih.gov/pubmed/24664114
http://dx.doi.org/10.1371/journal.pone.0092801
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