High-Throughput Characterization of Blood Serum Proteomics of IBD Patients with Respect to Aging and Genetic Factors

To date, no large scale, systematic description of the blood serum proteome has been performed in inflammatory bowel disease (IBD) patients. By using microarray technology, a more complete description of the blood proteome of IBD patients is feasible. It may help to achieve a better understanding of...

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Autores principales: Di Narzo, Antonio F., Telesco, Shannon E., Brodmerkel, Carrie, Argmann, Carmen, Peters, Lauren A., Li, Katherine, Kidd, Brian, Dudley, Joel, Cho, Judy, Schadt, Eric E., Kasarskis, Andrew, Dobrin, Radu, Hao, Ke
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2017
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5271178/
https://www.ncbi.nlm.nih.gov/pubmed/28129359
http://dx.doi.org/10.1371/journal.pgen.1006565
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author Di Narzo, Antonio F.
Telesco, Shannon E.
Brodmerkel, Carrie
Argmann, Carmen
Peters, Lauren A.
Li, Katherine
Kidd, Brian
Dudley, Joel
Cho, Judy
Schadt, Eric E.
Kasarskis, Andrew
Dobrin, Radu
Hao, Ke
author_facet Di Narzo, Antonio F.
Telesco, Shannon E.
Brodmerkel, Carrie
Argmann, Carmen
Peters, Lauren A.
Li, Katherine
Kidd, Brian
Dudley, Joel
Cho, Judy
Schadt, Eric E.
Kasarskis, Andrew
Dobrin, Radu
Hao, Ke
author_sort Di Narzo, Antonio F.
collection PubMed
description To date, no large scale, systematic description of the blood serum proteome has been performed in inflammatory bowel disease (IBD) patients. By using microarray technology, a more complete description of the blood proteome of IBD patients is feasible. It may help to achieve a better understanding of the disease. We analyzed blood serum profiles of 1128 proteins in IBD patients of European descent (84 Crohn’s Disease (CD) subjects and 88 Ulcerative Colitis (UC) subjects) as well as 15 healthy control subjects, and linked protein variability to patient age (all cohorts) and genetic components (genotype data generated from CD patients). We discovered new, previously unreported aging-associated proteomic traits (such as serum Albumin level), confirmed previously reported results from different tissues (i.e., upregulation of APOE with aging), and found loss of regulation of MMP7 in CD patients. In carrying out a genome wide genotype-protein association study (proteomic Quantitative Trait Loci, pQTL) within the CD patients, we identified 41 distinct proteomic traits influenced by cis pQTLs (underlying SNPs are referred to as pSNPs). Significant overlaps between pQTLs and cis eQTLs corresponding to the same gene were observed and in some cases the QTL were related to inflammatory disease susceptibility. Importantly, we discovered that serum protein levels of MST1 (Macrophage Stimulating 1) were regulated by SNP rs3197999 (p = 5.96E-10, FDR<5%), an accepted GWAS locus for IBD. Filling the knowledge gap of molecular mechanisms between GWAS hits and disease susceptibility requires systematically dissecting the impact of the locus at the cell, mRNA expression, and protein levels. The technology and analysis tools that are now available for large-scale molecular studies can elucidate how alterations in the proteome driven by genetic polymorphisms cause or provide protection against disease. Herein, we demonstrated this directly by integrating proteomic and pQTLs with existing GWAS, mRNA expression, and eQTL datasets to provide insights into the biological processes underlying IBD and pinpoint causal genetic variants along with their downstream molecular consequences.
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spelling pubmed-52711782017-02-06 High-Throughput Characterization of Blood Serum Proteomics of IBD Patients with Respect to Aging and Genetic Factors Di Narzo, Antonio F. Telesco, Shannon E. Brodmerkel, Carrie Argmann, Carmen Peters, Lauren A. Li, Katherine Kidd, Brian Dudley, Joel Cho, Judy Schadt, Eric E. Kasarskis, Andrew Dobrin, Radu Hao, Ke PLoS Genet Research Article To date, no large scale, systematic description of the blood serum proteome has been performed in inflammatory bowel disease (IBD) patients. By using microarray technology, a more complete description of the blood proteome of IBD patients is feasible. It may help to achieve a better understanding of the disease. We analyzed blood serum profiles of 1128 proteins in IBD patients of European descent (84 Crohn’s Disease (CD) subjects and 88 Ulcerative Colitis (UC) subjects) as well as 15 healthy control subjects, and linked protein variability to patient age (all cohorts) and genetic components (genotype data generated from CD patients). We discovered new, previously unreported aging-associated proteomic traits (such as serum Albumin level), confirmed previously reported results from different tissues (i.e., upregulation of APOE with aging), and found loss of regulation of MMP7 in CD patients. In carrying out a genome wide genotype-protein association study (proteomic Quantitative Trait Loci, pQTL) within the CD patients, we identified 41 distinct proteomic traits influenced by cis pQTLs (underlying SNPs are referred to as pSNPs). Significant overlaps between pQTLs and cis eQTLs corresponding to the same gene were observed and in some cases the QTL were related to inflammatory disease susceptibility. Importantly, we discovered that serum protein levels of MST1 (Macrophage Stimulating 1) were regulated by SNP rs3197999 (p = 5.96E-10, FDR<5%), an accepted GWAS locus for IBD. Filling the knowledge gap of molecular mechanisms between GWAS hits and disease susceptibility requires systematically dissecting the impact of the locus at the cell, mRNA expression, and protein levels. The technology and analysis tools that are now available for large-scale molecular studies can elucidate how alterations in the proteome driven by genetic polymorphisms cause or provide protection against disease. Herein, we demonstrated this directly by integrating proteomic and pQTLs with existing GWAS, mRNA expression, and eQTL datasets to provide insights into the biological processes underlying IBD and pinpoint causal genetic variants along with their downstream molecular consequences. Public Library of Science 2017-01-27 /pmc/articles/PMC5271178/ /pubmed/28129359 http://dx.doi.org/10.1371/journal.pgen.1006565 Text en © 2017 Di Narzo 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 (http://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
Di Narzo, Antonio F.
Telesco, Shannon E.
Brodmerkel, Carrie
Argmann, Carmen
Peters, Lauren A.
Li, Katherine
Kidd, Brian
Dudley, Joel
Cho, Judy
Schadt, Eric E.
Kasarskis, Andrew
Dobrin, Radu
Hao, Ke
High-Throughput Characterization of Blood Serum Proteomics of IBD Patients with Respect to Aging and Genetic Factors
title High-Throughput Characterization of Blood Serum Proteomics of IBD Patients with Respect to Aging and Genetic Factors
title_full High-Throughput Characterization of Blood Serum Proteomics of IBD Patients with Respect to Aging and Genetic Factors
title_fullStr High-Throughput Characterization of Blood Serum Proteomics of IBD Patients with Respect to Aging and Genetic Factors
title_full_unstemmed High-Throughput Characterization of Blood Serum Proteomics of IBD Patients with Respect to Aging and Genetic Factors
title_short High-Throughput Characterization of Blood Serum Proteomics of IBD Patients with Respect to Aging and Genetic Factors
title_sort high-throughput characterization of blood serum proteomics of ibd patients with respect to aging and genetic factors
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5271178/
https://www.ncbi.nlm.nih.gov/pubmed/28129359
http://dx.doi.org/10.1371/journal.pgen.1006565
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