Cargando…
Multi-Organ Expression Profiling Uncovers a Gene Module in Coronary Artery Disease Involving Transendothelial Migration of Leukocytes and LIM Domain Binding 2: The Stockholm Atherosclerosis Gene Expression (STAGE) Study
Environmental exposures filtered through the genetic make-up of each individual alter the transcriptional repertoire in organs central to metabolic homeostasis, thereby affecting arterial lipid accumulation, inflammation, and the development of coronary artery disease (CAD). The primary aim of the S...
| Autores principales: | , , , , , , , , , , , , , , , , , , , , , , , , , , , |
|---|---|
| Formato: | Texto |
| Lenguaje: | English |
| Publicado: |
Public Library of Science
2009
|
| Materias: | |
| Acceso en línea: | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2780352/ https://www.ncbi.nlm.nih.gov/pubmed/19997623 http://dx.doi.org/10.1371/journal.pgen.1000754 |
| _version_ | 1782174471234256896 |
|---|---|
| author | Hägg, Sara Skogsberg, Josefin Lundström, Jesper Noori, Peri Nilsson, Roland Zhong, Hua Maleki, Shohreh Shang, Ming-Mei Brinne, Björn Bradshaw, Maria Bajic, Vladimir B. Samnegård, Ann Silveira, Angela Kaplan, Lee M. Gigante, Bruna Leander, Karin de Faire, Ulf Rosfors, Stefan Lockowandt, Ulf Liska, Jan Konrad, Peter Takolander, Rabbe Franco-Cereceda, Anders Schadt, Eric E. Ivert, Torbjörn Hamsten, Anders Tegnér, Jesper Björkegren, Johan |
| author_facet | Hägg, Sara Skogsberg, Josefin Lundström, Jesper Noori, Peri Nilsson, Roland Zhong, Hua Maleki, Shohreh Shang, Ming-Mei Brinne, Björn Bradshaw, Maria Bajic, Vladimir B. Samnegård, Ann Silveira, Angela Kaplan, Lee M. Gigante, Bruna Leander, Karin de Faire, Ulf Rosfors, Stefan Lockowandt, Ulf Liska, Jan Konrad, Peter Takolander, Rabbe Franco-Cereceda, Anders Schadt, Eric E. Ivert, Torbjörn Hamsten, Anders Tegnér, Jesper Björkegren, Johan |
| author_sort | Hägg, Sara |
| collection | PubMed |
| description | Environmental exposures filtered through the genetic make-up of each individual alter the transcriptional repertoire in organs central to metabolic homeostasis, thereby affecting arterial lipid accumulation, inflammation, and the development of coronary artery disease (CAD). The primary aim of the Stockholm Atherosclerosis Gene Expression (STAGE) study was to determine whether there are functionally associated genes (rather than individual genes) important for CAD development. To this end, two-way clustering was used on 278 transcriptional profiles of liver, skeletal muscle, and visceral fat (n = 66/tissue) and atherosclerotic and unaffected arterial wall (n = 40/tissue) isolated from CAD patients during coronary artery bypass surgery. The first step, across all mRNA signals (n = 15,042/12,621 RefSeqs/genes) in each tissue, resulted in a total of 60 tissue clusters (n = 3958 genes). In the second step (performed within tissue clusters), one atherosclerotic lesion (n = 49/48) and one visceral fat (n = 59) cluster segregated the patients into two groups that differed in the extent of coronary stenosis (P = 0.008 and P = 0.00015). The associations of these clusters with coronary atherosclerosis were validated by analyzing carotid atherosclerosis expression profiles. Remarkably, in one cluster (n = 55/54) relating to carotid stenosis (P = 0.04), 27 genes in the two clusters relating to coronary stenosis were confirmed (n = 16/17, P<10(−27and−30)). Genes in the transendothelial migration of leukocytes (TEML) pathway were overrepresented in all three clusters, referred to as the atherosclerosis module (A-module). In a second validation step, using three independent cohorts, the A-module was found to be genetically enriched with CAD risk by 1.8-fold (P<0.004). The transcription co-factor LIM domain binding 2 (LDB2) was identified as a potential high-hierarchy regulator of the A-module, a notion supported by subnetwork analysis, by cellular and lesion expression of LDB2, and by the expression of 13 TEML genes in Ldb2–deficient arterial wall. Thus, the A-module appears to be important for atherosclerosis development and, together with LDB2, merits further attention in CAD research. |
| format | Text |
| id | pubmed-2780352 |
| institution | National Center for Biotechnology Information |
| language | English |
| publishDate | 2009 |
| publisher | Public Library of Science |
| record_format | MEDLINE/PubMed |
| spelling | pubmed-27803522009-12-08 Multi-Organ Expression Profiling Uncovers a Gene Module in Coronary Artery Disease Involving Transendothelial Migration of Leukocytes and LIM Domain Binding 2: The Stockholm Atherosclerosis Gene Expression (STAGE) Study Hägg, Sara Skogsberg, Josefin Lundström, Jesper Noori, Peri Nilsson, Roland Zhong, Hua Maleki, Shohreh Shang, Ming-Mei Brinne, Björn Bradshaw, Maria Bajic, Vladimir B. Samnegård, Ann Silveira, Angela Kaplan, Lee M. Gigante, Bruna Leander, Karin de Faire, Ulf Rosfors, Stefan Lockowandt, Ulf Liska, Jan Konrad, Peter Takolander, Rabbe Franco-Cereceda, Anders Schadt, Eric E. Ivert, Torbjörn Hamsten, Anders Tegnér, Jesper Björkegren, Johan PLoS Genet Research Article Environmental exposures filtered through the genetic make-up of each individual alter the transcriptional repertoire in organs central to metabolic homeostasis, thereby affecting arterial lipid accumulation, inflammation, and the development of coronary artery disease (CAD). The primary aim of the Stockholm Atherosclerosis Gene Expression (STAGE) study was to determine whether there are functionally associated genes (rather than individual genes) important for CAD development. To this end, two-way clustering was used on 278 transcriptional profiles of liver, skeletal muscle, and visceral fat (n = 66/tissue) and atherosclerotic and unaffected arterial wall (n = 40/tissue) isolated from CAD patients during coronary artery bypass surgery. The first step, across all mRNA signals (n = 15,042/12,621 RefSeqs/genes) in each tissue, resulted in a total of 60 tissue clusters (n = 3958 genes). In the second step (performed within tissue clusters), one atherosclerotic lesion (n = 49/48) and one visceral fat (n = 59) cluster segregated the patients into two groups that differed in the extent of coronary stenosis (P = 0.008 and P = 0.00015). The associations of these clusters with coronary atherosclerosis were validated by analyzing carotid atherosclerosis expression profiles. Remarkably, in one cluster (n = 55/54) relating to carotid stenosis (P = 0.04), 27 genes in the two clusters relating to coronary stenosis were confirmed (n = 16/17, P<10(−27and−30)). Genes in the transendothelial migration of leukocytes (TEML) pathway were overrepresented in all three clusters, referred to as the atherosclerosis module (A-module). In a second validation step, using three independent cohorts, the A-module was found to be genetically enriched with CAD risk by 1.8-fold (P<0.004). The transcription co-factor LIM domain binding 2 (LDB2) was identified as a potential high-hierarchy regulator of the A-module, a notion supported by subnetwork analysis, by cellular and lesion expression of LDB2, and by the expression of 13 TEML genes in Ldb2–deficient arterial wall. Thus, the A-module appears to be important for atherosclerosis development and, together with LDB2, merits further attention in CAD research. Public Library of Science 2009-12-04 /pmc/articles/PMC2780352/ /pubmed/19997623 http://dx.doi.org/10.1371/journal.pgen.1000754 Text en Hägg 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 Hägg, Sara Skogsberg, Josefin Lundström, Jesper Noori, Peri Nilsson, Roland Zhong, Hua Maleki, Shohreh Shang, Ming-Mei Brinne, Björn Bradshaw, Maria Bajic, Vladimir B. Samnegård, Ann Silveira, Angela Kaplan, Lee M. Gigante, Bruna Leander, Karin de Faire, Ulf Rosfors, Stefan Lockowandt, Ulf Liska, Jan Konrad, Peter Takolander, Rabbe Franco-Cereceda, Anders Schadt, Eric E. Ivert, Torbjörn Hamsten, Anders Tegnér, Jesper Björkegren, Johan Multi-Organ Expression Profiling Uncovers a Gene Module in Coronary Artery Disease Involving Transendothelial Migration of Leukocytes and LIM Domain Binding 2: The Stockholm Atherosclerosis Gene Expression (STAGE) Study |
| title | Multi-Organ Expression Profiling Uncovers a Gene Module in Coronary Artery Disease Involving Transendothelial Migration of Leukocytes and LIM Domain Binding 2: The Stockholm Atherosclerosis Gene Expression (STAGE) Study |
| title_full | Multi-Organ Expression Profiling Uncovers a Gene Module in Coronary Artery Disease Involving Transendothelial Migration of Leukocytes and LIM Domain Binding 2: The Stockholm Atherosclerosis Gene Expression (STAGE) Study |
| title_fullStr | Multi-Organ Expression Profiling Uncovers a Gene Module in Coronary Artery Disease Involving Transendothelial Migration of Leukocytes and LIM Domain Binding 2: The Stockholm Atherosclerosis Gene Expression (STAGE) Study |
| title_full_unstemmed | Multi-Organ Expression Profiling Uncovers a Gene Module in Coronary Artery Disease Involving Transendothelial Migration of Leukocytes and LIM Domain Binding 2: The Stockholm Atherosclerosis Gene Expression (STAGE) Study |
| title_short | Multi-Organ Expression Profiling Uncovers a Gene Module in Coronary Artery Disease Involving Transendothelial Migration of Leukocytes and LIM Domain Binding 2: The Stockholm Atherosclerosis Gene Expression (STAGE) Study |
| title_sort | multi-organ expression profiling uncovers a gene module in coronary artery disease involving transendothelial migration of leukocytes and lim domain binding 2: the stockholm atherosclerosis gene expression (stage) study |
| topic | Research Article |
| url | https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2780352/ https://www.ncbi.nlm.nih.gov/pubmed/19997623 http://dx.doi.org/10.1371/journal.pgen.1000754 |
| work_keys_str_mv | AT haggsara multiorganexpressionprofilinguncoversagenemoduleincoronaryarterydiseaseinvolvingtransendothelialmigrationofleukocytesandlimdomainbinding2thestockholmatherosclerosisgeneexpressionstagestudy AT skogsbergjosefin multiorganexpressionprofilinguncoversagenemoduleincoronaryarterydiseaseinvolvingtransendothelialmigrationofleukocytesandlimdomainbinding2thestockholmatherosclerosisgeneexpressionstagestudy AT lundstromjesper multiorganexpressionprofilinguncoversagenemoduleincoronaryarterydiseaseinvolvingtransendothelialmigrationofleukocytesandlimdomainbinding2thestockholmatherosclerosisgeneexpressionstagestudy AT nooriperi multiorganexpressionprofilinguncoversagenemoduleincoronaryarterydiseaseinvolvingtransendothelialmigrationofleukocytesandlimdomainbinding2thestockholmatherosclerosisgeneexpressionstagestudy AT nilssonroland multiorganexpressionprofilinguncoversagenemoduleincoronaryarterydiseaseinvolvingtransendothelialmigrationofleukocytesandlimdomainbinding2thestockholmatherosclerosisgeneexpressionstagestudy AT zhonghua multiorganexpressionprofilinguncoversagenemoduleincoronaryarterydiseaseinvolvingtransendothelialmigrationofleukocytesandlimdomainbinding2thestockholmatherosclerosisgeneexpressionstagestudy AT malekishohreh multiorganexpressionprofilinguncoversagenemoduleincoronaryarterydiseaseinvolvingtransendothelialmigrationofleukocytesandlimdomainbinding2thestockholmatherosclerosisgeneexpressionstagestudy AT shangmingmei multiorganexpressionprofilinguncoversagenemoduleincoronaryarterydiseaseinvolvingtransendothelialmigrationofleukocytesandlimdomainbinding2thestockholmatherosclerosisgeneexpressionstagestudy AT brinnebjorn multiorganexpressionprofilinguncoversagenemoduleincoronaryarterydiseaseinvolvingtransendothelialmigrationofleukocytesandlimdomainbinding2thestockholmatherosclerosisgeneexpressionstagestudy AT bradshawmaria multiorganexpressionprofilinguncoversagenemoduleincoronaryarterydiseaseinvolvingtransendothelialmigrationofleukocytesandlimdomainbinding2thestockholmatherosclerosisgeneexpressionstagestudy AT bajicvladimirb multiorganexpressionprofilinguncoversagenemoduleincoronaryarterydiseaseinvolvingtransendothelialmigrationofleukocytesandlimdomainbinding2thestockholmatherosclerosisgeneexpressionstagestudy AT samnegardann multiorganexpressionprofilinguncoversagenemoduleincoronaryarterydiseaseinvolvingtransendothelialmigrationofleukocytesandlimdomainbinding2thestockholmatherosclerosisgeneexpressionstagestudy AT silveiraangela multiorganexpressionprofilinguncoversagenemoduleincoronaryarterydiseaseinvolvingtransendothelialmigrationofleukocytesandlimdomainbinding2thestockholmatherosclerosisgeneexpressionstagestudy AT kaplanleem multiorganexpressionprofilinguncoversagenemoduleincoronaryarterydiseaseinvolvingtransendothelialmigrationofleukocytesandlimdomainbinding2thestockholmatherosclerosisgeneexpressionstagestudy AT gigantebruna multiorganexpressionprofilinguncoversagenemoduleincoronaryarterydiseaseinvolvingtransendothelialmigrationofleukocytesandlimdomainbinding2thestockholmatherosclerosisgeneexpressionstagestudy AT leanderkarin multiorganexpressionprofilinguncoversagenemoduleincoronaryarterydiseaseinvolvingtransendothelialmigrationofleukocytesandlimdomainbinding2thestockholmatherosclerosisgeneexpressionstagestudy AT defaireulf multiorganexpressionprofilinguncoversagenemoduleincoronaryarterydiseaseinvolvingtransendothelialmigrationofleukocytesandlimdomainbinding2thestockholmatherosclerosisgeneexpressionstagestudy AT rosforsstefan multiorganexpressionprofilinguncoversagenemoduleincoronaryarterydiseaseinvolvingtransendothelialmigrationofleukocytesandlimdomainbinding2thestockholmatherosclerosisgeneexpressionstagestudy AT lockowandtulf multiorganexpressionprofilinguncoversagenemoduleincoronaryarterydiseaseinvolvingtransendothelialmigrationofleukocytesandlimdomainbinding2thestockholmatherosclerosisgeneexpressionstagestudy AT liskajan multiorganexpressionprofilinguncoversagenemoduleincoronaryarterydiseaseinvolvingtransendothelialmigrationofleukocytesandlimdomainbinding2thestockholmatherosclerosisgeneexpressionstagestudy AT konradpeter multiorganexpressionprofilinguncoversagenemoduleincoronaryarterydiseaseinvolvingtransendothelialmigrationofleukocytesandlimdomainbinding2thestockholmatherosclerosisgeneexpressionstagestudy AT takolanderrabbe multiorganexpressionprofilinguncoversagenemoduleincoronaryarterydiseaseinvolvingtransendothelialmigrationofleukocytesandlimdomainbinding2thestockholmatherosclerosisgeneexpressionstagestudy AT francocerecedaanders multiorganexpressionprofilinguncoversagenemoduleincoronaryarterydiseaseinvolvingtransendothelialmigrationofleukocytesandlimdomainbinding2thestockholmatherosclerosisgeneexpressionstagestudy AT schadterice multiorganexpressionprofilinguncoversagenemoduleincoronaryarterydiseaseinvolvingtransendothelialmigrationofleukocytesandlimdomainbinding2thestockholmatherosclerosisgeneexpressionstagestudy AT iverttorbjorn multiorganexpressionprofilinguncoversagenemoduleincoronaryarterydiseaseinvolvingtransendothelialmigrationofleukocytesandlimdomainbinding2thestockholmatherosclerosisgeneexpressionstagestudy AT hamstenanders multiorganexpressionprofilinguncoversagenemoduleincoronaryarterydiseaseinvolvingtransendothelialmigrationofleukocytesandlimdomainbinding2thestockholmatherosclerosisgeneexpressionstagestudy AT tegnerjesper multiorganexpressionprofilinguncoversagenemoduleincoronaryarterydiseaseinvolvingtransendothelialmigrationofleukocytesandlimdomainbinding2thestockholmatherosclerosisgeneexpressionstagestudy AT bjorkegrenjohan multiorganexpressionprofilinguncoversagenemoduleincoronaryarterydiseaseinvolvingtransendothelialmigrationofleukocytesandlimdomainbinding2thestockholmatherosclerosisgeneexpressionstagestudy |