Whole Blood Transcriptomics in Cardiac Surgery Identifies a Gene Regulatory Network Connecting Ischemia Reperfusion with Systemic Inflammation

BACKGROUND: Cardiac surgery with cardiopulmonary bypass (CS/CPB) is associated with increased risk for postoperative complications causing substantial morbidity and mortality. To identify the molecular mechanisms underlying CS/CPB-induced pathophysiology we employed an integrative systems biology ap...

Descripción completa

Detalles Bibliográficos
Autores principales: Liangos, Orfeas, Domhan, Sophie, Schwager, Christian, Zeier, Martin, Huber, Peter E., Addabbo, Francesco, Goligorsky, Michael S., Hlatky, Lynn, Jaber, Bertrand L., Abdollahi, Amir
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2010
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2965092/
https://www.ncbi.nlm.nih.gov/pubmed/21048961
http://dx.doi.org/10.1371/journal.pone.0013658
_version_ 1782189468410707968
author Liangos, Orfeas
Domhan, Sophie
Schwager, Christian
Zeier, Martin
Huber, Peter E.
Addabbo, Francesco
Goligorsky, Michael S.
Hlatky, Lynn
Jaber, Bertrand L.
Abdollahi, Amir
author_facet Liangos, Orfeas
Domhan, Sophie
Schwager, Christian
Zeier, Martin
Huber, Peter E.
Addabbo, Francesco
Goligorsky, Michael S.
Hlatky, Lynn
Jaber, Bertrand L.
Abdollahi, Amir
author_sort Liangos, Orfeas
collection PubMed
description BACKGROUND: Cardiac surgery with cardiopulmonary bypass (CS/CPB) is associated with increased risk for postoperative complications causing substantial morbidity and mortality. To identify the molecular mechanisms underlying CS/CPB-induced pathophysiology we employed an integrative systems biology approach using the whole blood transcriptome as the sentinel organ. METHODOLOGY/PRINCIPAL FINDINGS: Total RNA was isolated and globin mRNA depleted from whole blood samples prospectively collected from 10 patients at time points prior (0), 2 and 24 hours following CS/CPB. Genome-wide transcriptional analysis revealed differential expression of 610 genes after CS/CPB (p<0.01). Among the 375 CS/CPB-upregulated genes, we found a gene-regulatory network consisting of 50 genes, reminiscent of activation of a coordinated genetic program triggered by CS/CPB. Intriguingly, the highly connected hub nodes of the identified network included key sensors of ischemia-reperfusion (HIF-1alpha and C/EBPbeta). Activation of this network initiated a concerted inflammatory response via upregulation of TLR-4/5, IL1R2/IL1RAP, IL6, IL18/IL18R1/IL18RAP, MMP9, HGF/HGFR, CalgranulinA/B, and coagulation factors F5/F12 among others. Differential regulation of 13 candidate genes including novel, not hitherto CS/CBP-associated genes, such as PTX3, PGK1 and Resistin, was confirmed using real-time quantitative RT-PCR. In support of the mRNA data, differential expression of MMP9, MIP1alpha and MIP1beta plasma proteins was further confirmed in 34 additional patients. CONCLUSIONS: Analysis of blood transcriptome uncovered critical signaling pathways governing the CS/CPB-induced pathophysiology. The molecular signaling underlying ischemia reperfusion and inflammatory response is highly intertwined and includes pro-inflammatory as well as cardioprotective elements. The herein identified candidate genes and pathways may provide promising prognostic biomarker and therapeutic targets.
format Text
id pubmed-2965092
institution National Center for Biotechnology Information
language English
publishDate 2010
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-29650922010-11-03 Whole Blood Transcriptomics in Cardiac Surgery Identifies a Gene Regulatory Network Connecting Ischemia Reperfusion with Systemic Inflammation Liangos, Orfeas Domhan, Sophie Schwager, Christian Zeier, Martin Huber, Peter E. Addabbo, Francesco Goligorsky, Michael S. Hlatky, Lynn Jaber, Bertrand L. Abdollahi, Amir PLoS One Research Article BACKGROUND: Cardiac surgery with cardiopulmonary bypass (CS/CPB) is associated with increased risk for postoperative complications causing substantial morbidity and mortality. To identify the molecular mechanisms underlying CS/CPB-induced pathophysiology we employed an integrative systems biology approach using the whole blood transcriptome as the sentinel organ. METHODOLOGY/PRINCIPAL FINDINGS: Total RNA was isolated and globin mRNA depleted from whole blood samples prospectively collected from 10 patients at time points prior (0), 2 and 24 hours following CS/CPB. Genome-wide transcriptional analysis revealed differential expression of 610 genes after CS/CPB (p<0.01). Among the 375 CS/CPB-upregulated genes, we found a gene-regulatory network consisting of 50 genes, reminiscent of activation of a coordinated genetic program triggered by CS/CPB. Intriguingly, the highly connected hub nodes of the identified network included key sensors of ischemia-reperfusion (HIF-1alpha and C/EBPbeta). Activation of this network initiated a concerted inflammatory response via upregulation of TLR-4/5, IL1R2/IL1RAP, IL6, IL18/IL18R1/IL18RAP, MMP9, HGF/HGFR, CalgranulinA/B, and coagulation factors F5/F12 among others. Differential regulation of 13 candidate genes including novel, not hitherto CS/CBP-associated genes, such as PTX3, PGK1 and Resistin, was confirmed using real-time quantitative RT-PCR. In support of the mRNA data, differential expression of MMP9, MIP1alpha and MIP1beta plasma proteins was further confirmed in 34 additional patients. CONCLUSIONS: Analysis of blood transcriptome uncovered critical signaling pathways governing the CS/CPB-induced pathophysiology. The molecular signaling underlying ischemia reperfusion and inflammatory response is highly intertwined and includes pro-inflammatory as well as cardioprotective elements. The herein identified candidate genes and pathways may provide promising prognostic biomarker and therapeutic targets. Public Library of Science 2010-10-27 /pmc/articles/PMC2965092/ /pubmed/21048961 http://dx.doi.org/10.1371/journal.pone.0013658 Text en Liangos 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
Liangos, Orfeas
Domhan, Sophie
Schwager, Christian
Zeier, Martin
Huber, Peter E.
Addabbo, Francesco
Goligorsky, Michael S.
Hlatky, Lynn
Jaber, Bertrand L.
Abdollahi, Amir
Whole Blood Transcriptomics in Cardiac Surgery Identifies a Gene Regulatory Network Connecting Ischemia Reperfusion with Systemic Inflammation
title Whole Blood Transcriptomics in Cardiac Surgery Identifies a Gene Regulatory Network Connecting Ischemia Reperfusion with Systemic Inflammation
title_full Whole Blood Transcriptomics in Cardiac Surgery Identifies a Gene Regulatory Network Connecting Ischemia Reperfusion with Systemic Inflammation
title_fullStr Whole Blood Transcriptomics in Cardiac Surgery Identifies a Gene Regulatory Network Connecting Ischemia Reperfusion with Systemic Inflammation
title_full_unstemmed Whole Blood Transcriptomics in Cardiac Surgery Identifies a Gene Regulatory Network Connecting Ischemia Reperfusion with Systemic Inflammation
title_short Whole Blood Transcriptomics in Cardiac Surgery Identifies a Gene Regulatory Network Connecting Ischemia Reperfusion with Systemic Inflammation
title_sort whole blood transcriptomics in cardiac surgery identifies a gene regulatory network connecting ischemia reperfusion with systemic inflammation
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2965092/
https://www.ncbi.nlm.nih.gov/pubmed/21048961
http://dx.doi.org/10.1371/journal.pone.0013658
work_keys_str_mv AT liangosorfeas wholebloodtranscriptomicsincardiacsurgeryidentifiesageneregulatorynetworkconnectingischemiareperfusionwithsystemicinflammation
AT domhansophie wholebloodtranscriptomicsincardiacsurgeryidentifiesageneregulatorynetworkconnectingischemiareperfusionwithsystemicinflammation
AT schwagerchristian wholebloodtranscriptomicsincardiacsurgeryidentifiesageneregulatorynetworkconnectingischemiareperfusionwithsystemicinflammation
AT zeiermartin wholebloodtranscriptomicsincardiacsurgeryidentifiesageneregulatorynetworkconnectingischemiareperfusionwithsystemicinflammation
AT huberpetere wholebloodtranscriptomicsincardiacsurgeryidentifiesageneregulatorynetworkconnectingischemiareperfusionwithsystemicinflammation
AT addabbofrancesco wholebloodtranscriptomicsincardiacsurgeryidentifiesageneregulatorynetworkconnectingischemiareperfusionwithsystemicinflammation
AT goligorskymichaels wholebloodtranscriptomicsincardiacsurgeryidentifiesageneregulatorynetworkconnectingischemiareperfusionwithsystemicinflammation
AT hlatkylynn wholebloodtranscriptomicsincardiacsurgeryidentifiesageneregulatorynetworkconnectingischemiareperfusionwithsystemicinflammation
AT jaberbertrandl wholebloodtranscriptomicsincardiacsurgeryidentifiesageneregulatorynetworkconnectingischemiareperfusionwithsystemicinflammation
AT abdollahiamir wholebloodtranscriptomicsincardiacsurgeryidentifiesageneregulatorynetworkconnectingischemiareperfusionwithsystemicinflammation

Ejemplares similares