DOT1L regulates chamber-specific transcriptional networks during cardiogenesis 
and mediates postnatal cell cycle withdrawal

Cattaneo, Paola; Hayes, Michael G. B.; Baumgarten, Nina; Hecker, Dennis; Peruzzo, Sofia; Aslan, Galip S.; Kunderfranco, Paolo; Larcher, Veronica; Zhang, Lunfeng; Contu, Riccardo; Fonseca, Gregory; Spinozzi, Simone; Chen, Ju; Condorelli, Gianluigi; Dimmeler, Stefanie; Schulz, Marcel H.; Heinz, Sven; Guimaraes-Camboa, Nuno; Evans, Sylvia M.

doi:10.1038/s41467-022-35070-2

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DOT1L regulates chamber-specific transcriptional networks during cardiogenesis and mediates postnatal cell cycle withdrawal

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Peruzzo, Sofia
Developmental Genetics, Max Planck Institute for Heart and Lung Research, Max Planck Society;

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Aslan, Galip S.
IMPRS, Max Planck Institute for Heart and Lung Research, Max Planck Society;

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Citation

Cattaneo, P., Hayes, M. G. B., Baumgarten, N., Hecker, D., Peruzzo, S., Aslan, G. S., et al. (2022). DOT1L regulates chamber-specific transcriptional networks during cardiogenesis and mediates postnatal cell cycle withdrawal. NATURE COMMUNICATIONS, 13(1): 7444. doi:10.1038/s41467-022-35070-2.

Cite as: https://hdl.handle.net/21.11116/0000-000C-CC7F-1

Abstract

Mechanisms by which specific histone modifications regulate distinct gene networks remain little understood. We investigated how H3K79me2, a modification catalyzed by DOT1L and previously considered a general transcriptional activation mark, regulates gene expression during cardiogenesis. Embryonic cardiomyocyte ablation of Dot1l revealed that H3K79me2 does not act as a general transcriptional activator, but rather regulates highly specific transcriptional networks at two critical cardiogenic junctures: embryonic cardiogenesis, where it was particularly important for left ventricle-specific genes, and postnatal cardiomyocyte cell cycle withdrawal, with Dot1L mutants having more mononuclear cardiomyocytes and prolonged cardiomyocyte cell cycle activity. Mechanistic analyses revealed that H3K79me2 in two distinct domains, gene bodies and regulatory elements, synergized to promote expression of genes activated by DOT1L. Surprisingly, H3K79me2 in specific regulatory elements also contributed to silencing genes usually not expressed in cardiomyocytes. These results reveal mechanisms by which DOT1L successively regulates left ventricle specification and cardiomyocyte cell cycle withdrawal. How and whether histone modifications regulate distinct gene networks remains insufficiently understood. Here Cattaneo et al show that DOT1L catalyzed H3K79me2 regulates fetal chamber-specific gene expression and neonatal cardiomyocyte cell cycle withdrawal to coordinate heart development.