Transcriptome analysis of human heart failure reveals dysregulated cell adhesion in dilated cardiomyopathy and activated immune pathways in ischemic heart failure

Mary E. Sweet; Andrea Cocciolo; Dobromir Slavov; Kenneth L. Jones; Joseph R. Sweet; Sharon L. Graw; T. Brett Reece; Amrut V. Ambardekar; Michael R. Bristow; Luisa Mestroni; Matthew R. G. Taylor

doi:10.1186/s12864-018-5213-9

BMC Genomics (Nov 2018)

Transcriptome analysis of human heart failure reveals dysregulated cell adhesion in dilated cardiomyopathy and activated immune pathways in ischemic heart failure

Mary E. Sweet,
Andrea Cocciolo,
Dobromir Slavov,
Kenneth L. Jones,
Joseph R. Sweet,
Sharon L. Graw,
T. Brett Reece,
Amrut V. Ambardekar,
Michael R. Bristow,
Luisa Mestroni,
Matthew R. G. Taylor

Affiliations

Mary E. Sweet: Human Medical Genetics and Genomics, University of Colorado
Andrea Cocciolo: Cardiovascular Institute and Adult Medical Genetics Program, University of Colorado
Dobromir Slavov: Cardiovascular Institute and Adult Medical Genetics Program, University of Colorado
Kenneth L. Jones: Department of Pediatrics, Section of Hematology, Oncology, and Bone Marrow Transplant, University of Colorado
Joseph R. Sweet: Department of Statistics, E. & J. Gallo
Sharon L. Graw: Cardiovascular Institute and Adult Medical Genetics Program, University of Colorado
T. Brett Reece: Department of Cardiothoracic Surgery, University of Colorado Hospital
Amrut V. Ambardekar: Division of Cardiology, Department of Medicine, University of Colorado
Michael R. Bristow: Division of Cardiology, Department of Medicine, University of Colorado
Luisa Mestroni: Human Medical Genetics and Genomics, University of Colorado
Matthew R. G. Taylor: Human Medical Genetics and Genomics, University of Colorado

DOI: https://doi.org/10.1186/s12864-018-5213-9
Journal volume & issue: Vol. 19, no. 1
pp. 1 – 14

Abstract

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Abstract Background Current heart failure (HF) treatment is based on targeting symptoms and left ventricle dysfunction severity, relying on a common HF pathway paradigm to justify common treatments for HF patients. This common strategy may belie an incomplete understanding of heterogeneous underlying mechanisms and could be a barrier to more precise treatments. We hypothesized we could use RNA-sequencing (RNA-seq) in human heart tissue to delineate HF etiology-specific gene expression signatures. Results RNA-seq from 64 human left ventricular samples: 37 dilated (DCM), 13 ischemic (ICM), and 14 non-failing (NF). Using a multi-analytic approach including covariate adjustment for age and sex, differentially expressed genes (DEGs) were identified characterizing HF and disease-specific expression. Pathway analysis investigated enrichment for biologically relevant pathways and functions. DCM vs NF and ICM vs NF had shared HF-DEGs that were enriched for the fetal gene program and mitochondrial dysfunction. DCM-specific DEGs were enriched for cell-cell and cell-matrix adhesion pathways. ICM-specific DEGs were enriched for cytoskeletal and immune pathway activation. Using the ICM and DCM DEG signatures from our data we were able to correctly classify the phenotypes of 24/31 ICM and 32/36 DCM samples from publicly available replication datasets. Conclusions Our results demonstrate the commonality of mitochondrial dysfunction in end-stage HF but more importantly reveal key etiology-specific signatures. Dysfunctional cell-cell and cell-matrix adhesion signatures typified DCM whereas signals related to immune and fibrotic responses were seen in ICM. These findings suggest that transcriptome signatures may distinguish end-stage heart failure, shedding light on underlying biological differences between ICM and DCM.

Published in BMC Genomics

ISSN: 1471-2164 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Technology: Chemical technology: Biotechnology; Science: Biology (General): Genetics
Website: http://bmcgenomics.biomedcentral.com

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Abstract

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