RNAseq analysis of heart tissue from mice treated with atenolol and isoproterenol reveals a reciprocal transcriptional response

Journal Article

2016

Permanent link to this Item
http://hdl.handle.net/11427/34262
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BergmannSven_RNAseq_analysis_2016.pdf (3.01 MB)
Authors
Bergmann, Sven
Journal Title

BMC Genomics

Link to Journal
https://dx.doi.org/10.1186/s12864-016-3059-6
Journal ISSN
Volume Title
Publisher
Publisher
Department
Department of Integrative Biomedical Sciences (IBMS)
Faculty
Faculty of Health Sciences
License
Series
Abstract
Abstract Background The transcriptional response to many widely used drugs and its modulation by genetic variability is poorly understood. Here we present an analysis of RNAseq profiles from heart tissue of 18 inbred mouse strains treated with the β-blocker atenolol (ATE) and the β-agonist isoproterenol (ISO). Results Differential expression analyses revealed a large set of genes responding to ISO (n = 1770 at FDR = 0.0001) and a comparatively small one responding to ATE (n = 23 at FDR = 0.0001). At a less stringent definition of differential expression, the transcriptional responses to these two antagonistic drugs are reciprocal for many genes, with an overall anti-correlation of r = −0.3. This trend is also observed at the level of most individual strains even though the power to detect differential expression is significantly reduced. The inversely expressed gene sets are enriched with genes annotated for heart-related functions. Modular analysis revealed gene sets that exhibit coherent transcription profiles across some strains and/or treatments. Correlations between these modules and a broad spectrum of cardiovascular traits are stronger than expected by chance. This provides evidence for the overall importance of transcriptional regulation for these organismal responses and explicits links between co-expressed genes and the traits they are associated with. Gene set enrichment analysis of differentially expressed groups of genes pointed to pathways related to heart development and functionality. Conclusions Our study provides new insights into the transcriptional response of the heart to perturbations of the β-adrenergic system, implicating several new genes that had not been associated to this system previously.
Description
Keywords
Atenolol
Cardiac hypertrophy
Gene Expression Regulation
Gene Ontology
Gene Regulatory Networks
Heart
Isoproterenol
Mice
Mice, Inbred Strains
Sequence Analysis, RNA
Software
Isoproterenol
Mouse heart
RNAseq
β-adrenergic system
Animals
Atenolol
Computational Biology
Gene Expression Profiling

Reference:

Bergmann, S. 2016. RNAseq analysis of heart tissue from mice treated with atenolol and isoproterenol reveals a reciprocal transcriptional response. BMC Genomics. 17(1):174 - 177. http://hdl.handle.net/11427/34262

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