HDAC4 controls histone methylation in response to elevated cardiac load
Mathias Hohl, … , Johannes Backs, Christoph Maack
Mathias Hohl, … , Johannes Backs, Christoph Maack
Published February 22, 2013
Citation Information: J Clin Invest. 2013;123(3):1359-1370. https://doi.org/10.1172/JCI61084.
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Research Article Cardiology

HDAC4 controls histone methylation in response to elevated cardiac load

Abstract

In patients with heart failure, reactivation of a fetal gene program, including atrial natriuretic peptide (ANP) and brain natriuretic peptide (BNP), is a hallmark for maladaptive remodeling of the LV. The mechanisms that regulate this reactivation are incompletely understood. Histone acetylation and methylation affect the conformation of chromatin, which in turn governs the accessibility of DNA for transcription factors. Using human LV myocardium, we found that, despite nuclear export of histone deacetylase 4 (HDAC4), upregulation of ANP and BNP in failing hearts did not require increased histone acetylation in the promoter regions of these genes. In contrast, di- and trimethylation of lysine 9 of histone 3 (H3K9) and binding of heterochromatin protein 1 (HP1) in the promoter regions of these genes were substantially reduced. In isolated working murine hearts, an acute increase of cardiac preload induced HDAC4 nuclear export, H3K9 demethylation, HP1 dissociation from the promoter region, and activation of the ANP gene. These processes were reversed in hearts with myocyte-specific deletion of Hdac4. We conclude that HDAC4 plays a central role for rapid modifications of histone methylation in response to variations in cardiac load and may represent a target for pharmacological interventions to prevent maladaptive remodeling in patients with heart failure.

Authors

Mathias Hohl, Michael Wagner, Jan-Christian Reil, Sarah-Anne Müller, Marcus Tauchnitz, Angela M. Zimmer, Lorenz H. Lehmann, Gerald Thiel, Michael Böhm, Johannes Backs, Christoph Maack

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Figure 5

Increased nucleo-cytoplasmic shuttling of HDAC4 in failing myocardium.

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Increased nucleo-cytoplasmic shuttling of HDAC4 in failing myocardium. R...
Representative (A) and cumulative (B) results of Western blot analyses of HDAC4, mRNA polymerase II (Pol. II), and GAPDH in cytosolic (C) and nuclear (N) protein fractions of human nonfailing (n = 8) and failing (n = 16) myocardium. Nuclear protein expression was related to mRNA polymerase II, while cytosolic expression was related to GAPDH. Nucleo-cytoplasmic shuttling of HDAC4 was quantified by the cytosolic/nuclear ratio of HDAC4 expression (C). Correlation of nucleo-cytoplasmic shuttling of HDAC4 with H3K9me2 at ANP and BNP promoter regions (D) and ANP and BNP expression (E) in nonfailing and failing myocardium. ***P < 0.001, cytosolic vs. nuclear; P < 0.001, failing vs. nonfailing.