Dynamic Chromatin Targeting of BRD4 Stimulates Cardiac Fibroblast Activation

Matthew S Stratton; Rushita A Bagchi; Marina B Felisbino; Rachel A Hirsch; Harrison E Smith; Andrew S Riching; Blake Y Enyart; Keith A Koch; Maria A Cavasin; Michael Alexanian; Kunhua Song; Jun Qi; Madeleine E Lemieux; Deepak Srivastava; Maggie P Y Lam; Saptarsi M Haldar; Charles Y Lin; Timothy A McKinsey

doi:10.1161/CIRCRESAHA.119.315125

Dynamic Chromatin Targeting of BRD4 Stimulates Cardiac Fibroblast Activation

Circ Res. 2019 Sep 13;125(7):662-677. doi: 10.1161/CIRCRESAHA.119.315125. Epub 2019 Aug 14.

Authors

Matthew S Stratton^{1

2}, Rushita A Bagchi^{1

2}, Marina B Felisbino^{1

2}, Rachel A Hirsch³, Harrison E Smith³, Andrew S Riching^{1

2}, Blake Y Enyart^{1

2}, Keith A Koch^{1

2}, Maria A Cavasin^{1

2}, Michael Alexanian⁴, Kunhua Song^{1

2}, Jun Qi⁵, Madeleine E Lemieux⁶, Deepak Srivastava⁴, Maggie P Y Lam^{1

2}, Saptarsi M Haldar^{4

7

8}, Charles Y Lin³, Timothy A McKinsey^{1

2}

Affiliations

¹ From the Department of Medicine, Division of Cardiology (M.S.S., R.A.B., M.B.F., A.S.R., B.Y.E., K.A.K., M.A.C., K.S., M.P.Y.L., T.A.M.), University of Colorado Anschutz Medical Campus, Aurora.
² Consortium for Fibrosis Research & Translation (M.S.S., R.A.B., M.B.F., A.S.R., B.Y.E., K.A.K., M.A.C., K.S., M.P.Y.L., T.A.M.), University of Colorado Anschutz Medical Campus, Aurora.
³ Department of Molecular and Human Genetics, Baylor College of Medicine, Houston, TX (R.A.H., H.E.S., C.Y.L.).
⁴ Gladstone Institute of Cardiovascular Disease, San Francisco, CA (M.A., D.S., S.M.H.).
⁵ Department of Medical Oncology, Dana Farber Cancer Institute, Boston, MA (J.Q.).
⁶ Bioinfo, Plantagenet, ON, Canada (M.E.L.).
⁷ Cardiovascular Research Institute and Department of Medicine, Division of Cardiology UCSF School of Medicine, San Francisco, CA (S.M.H.).
⁸ Cardiometabolic Disorders, Amgen, San Francisco, CA (S.M.H.).

Abstract

Rationale: Small molecule inhibitors of the acetyl-histone binding protein BRD4 have been shown to block cardiac fibrosis in preclinical models of heart failure (HF). However, since the inhibitors target BRD4 ubiquitously, it is unclear whether this chromatin reader protein functions in cell type-specific manner to control pathological myocardial fibrosis. Furthermore, the molecular mechanisms by which BRD4 stimulates the transcriptional program for cardiac fibrosis remain unknown.

Objective: We sought to test the hypothesis that BRD4 functions in a cell-autonomous and signal-responsive manner to control activation of cardiac fibroblasts, which are the major extracellular matrix-producing cells of the heart.

Methods and results: RNA-sequencing, mass spectrometry, and cell-based assays employing primary adult rat ventricular fibroblasts demonstrated that BRD4 functions as an effector of TGF-β (transforming growth factor-β) signaling to stimulate conversion of quiescent cardiac fibroblasts into Periostin (Postn)-positive cells that express high levels of extracellular matrix. These findings were confirmed in vivo through whole-transcriptome analysis of cardiac fibroblasts from mice subjected to transverse aortic constriction and treated with the small molecule BRD4 inhibitor, JQ1. Chromatin immunoprecipitation-sequencing revealed that BRD4 undergoes stimulus-dependent, genome-wide redistribution in cardiac fibroblasts, becoming enriched on a subset of enhancers and super-enhancers, and leading to RNA polymerase II activation and expression of downstream target genes. Employing the Sertad4 (SERTA domain-containing protein 4) locus as a prototype, we demonstrate that dynamic chromatin targeting of BRD4 is controlled, in part, by p38 MAPK (mitogen-activated protein kinase) and provide evidence of a critical function for Sertad4 in TGF-β-mediated cardiac fibroblast activation.

Conclusions: These findings define BRD4 as a central regulator of the pro-fibrotic cardiac fibroblast phenotype, establish a p38-dependent signaling circuit for epigenetic reprogramming in heart failure, and uncover a novel role for Sertad4. The work provides a mechanistic foundation for the development of BRD4 inhibitors as targeted anti-fibrotic therapies for the heart.

Keywords: chromatin; fibroblast; heart failure; mass spectrometry; phenotype; signaling.

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Animals
Azepines / pharmacology
Azepines / therapeutic use
Cell Adhesion Molecules / genetics
Cell Adhesion Molecules / metabolism
Cells, Cultured
Chromatin / metabolism*
Enhancer Elements, Genetic
Epigenesis, Genetic
Extracellular Matrix / metabolism
Female
Fibrosis
Heart Failure / drug therapy
Heart Failure / genetics
Heart Failure / metabolism*
Heart Ventricles / cytology
Heart Ventricles / metabolism
Heart Ventricles / pathology
Intracellular Signaling Peptides and Proteins / antagonists & inhibitors
Intracellular Signaling Peptides and Proteins / genetics
Intracellular Signaling Peptides and Proteins / metabolism*
Male
Mice
Mice, Inbred C57BL
Myofibroblasts / metabolism*
Nuclear Proteins / antagonists & inhibitors
Nuclear Proteins / genetics
Nuclear Proteins / metabolism*
Protein Binding
RNA Polymerase II / metabolism
Rats
Rats, Sprague-Dawley
Transcription Factors / antagonists & inhibitors
Transcription Factors / genetics
Transcription Factors / metabolism*
Transcriptome
Transforming Growth Factor beta / genetics
Transforming Growth Factor beta / metabolism
Triazoles / pharmacology
Triazoles / therapeutic use
p38 Mitogen-Activated Protein Kinases / metabolism

Substances

(+)-JQ1 compound
Azepines
Brd4 protein, mouse
Cell Adhesion Molecules
Chromatin
Intracellular Signaling Peptides and Proteins
Nuclear Proteins
Postn protein, mouse
Sertad4 protein, mouse
Transcription Factors
Transforming Growth Factor beta
Triazoles
p38 Mitogen-Activated Protein Kinases
RNA Polymerase II

Abstract

Publication types

MeSH terms

Substances

Grants and funding