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Dynamic Competing Histone H4 K5K8 Acetylation and Butyrylation Are Hallmarks of Highly Active Gene Promoters

Recently discovered histone lysine acylation marks increase the functional diversity of nucleosomes well beyond acetylation. Here, we focus on histone butyrylation in the context of sperm cell differentiation. Specifically, we investigate the butyrylation of histone H4 lysine 5 and 8 at gene promote...

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Autores principales: Goudarzi, Afsaneh, Zhang, Di, Huang, He, Barral, Sophie, Kwon, Oh Kwang, Qi, Shankang, Tang, Zhanyun, Buchou, Thierry, Vitte, Anne-Laure, He, Tieming, Cheng, Zhongyi, Montellier, Emilie, Gaucher, Jonathan, Curtet, Sandrine, Debernardi, Alexandra, Charbonnier, Guillaume, Puthier, Denis, Petosa, Carlo, Panne, Daniel, Rousseaux, Sophie, Roeder, Robert G., Zhao, Yingming, Khochbin, Saadi
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Cell Press 2016
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4850424/
https://www.ncbi.nlm.nih.gov/pubmed/27105113
http://dx.doi.org/10.1016/j.molcel.2016.03.014
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author Goudarzi, Afsaneh
Zhang, Di
Huang, He
Barral, Sophie
Kwon, Oh Kwang
Qi, Shankang
Tang, Zhanyun
Buchou, Thierry
Vitte, Anne-Laure
He, Tieming
Cheng, Zhongyi
Montellier, Emilie
Gaucher, Jonathan
Curtet, Sandrine
Debernardi, Alexandra
Charbonnier, Guillaume
Puthier, Denis
Petosa, Carlo
Panne, Daniel
Rousseaux, Sophie
Roeder, Robert G.
Zhao, Yingming
Khochbin, Saadi
author_facet Goudarzi, Afsaneh
Zhang, Di
Huang, He
Barral, Sophie
Kwon, Oh Kwang
Qi, Shankang
Tang, Zhanyun
Buchou, Thierry
Vitte, Anne-Laure
He, Tieming
Cheng, Zhongyi
Montellier, Emilie
Gaucher, Jonathan
Curtet, Sandrine
Debernardi, Alexandra
Charbonnier, Guillaume
Puthier, Denis
Petosa, Carlo
Panne, Daniel
Rousseaux, Sophie
Roeder, Robert G.
Zhao, Yingming
Khochbin, Saadi
author_sort Goudarzi, Afsaneh
collection PubMed
description Recently discovered histone lysine acylation marks increase the functional diversity of nucleosomes well beyond acetylation. Here, we focus on histone butyrylation in the context of sperm cell differentiation. Specifically, we investigate the butyrylation of histone H4 lysine 5 and 8 at gene promoters where acetylation guides the binding of Brdt, a bromodomain-containing protein, thereby mediating stage-specific gene expression programs and post-meiotic chromatin reorganization. Genome-wide mapping data show that highly active Brdt-bound gene promoters systematically harbor competing histone acetylation and butyrylation marks at H4 K5 and H4 K8. Despite acting as a direct stimulator of transcription, histone butyrylation competes with acetylation, especially at H4 K5, to prevent Brdt binding. Additionally, H4 K5K8 butyrylation also marks retarded histone removal during late spermatogenesis. Hence, alternating H4 acetylation and butyrylation, while sustaining direct gene activation and dynamic bromodomain binding, could impact the final male epigenome features.
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spelling pubmed-48504242016-05-06 Dynamic Competing Histone H4 K5K8 Acetylation and Butyrylation Are Hallmarks of Highly Active Gene Promoters Goudarzi, Afsaneh Zhang, Di Huang, He Barral, Sophie Kwon, Oh Kwang Qi, Shankang Tang, Zhanyun Buchou, Thierry Vitte, Anne-Laure He, Tieming Cheng, Zhongyi Montellier, Emilie Gaucher, Jonathan Curtet, Sandrine Debernardi, Alexandra Charbonnier, Guillaume Puthier, Denis Petosa, Carlo Panne, Daniel Rousseaux, Sophie Roeder, Robert G. Zhao, Yingming Khochbin, Saadi Mol Cell Article Recently discovered histone lysine acylation marks increase the functional diversity of nucleosomes well beyond acetylation. Here, we focus on histone butyrylation in the context of sperm cell differentiation. Specifically, we investigate the butyrylation of histone H4 lysine 5 and 8 at gene promoters where acetylation guides the binding of Brdt, a bromodomain-containing protein, thereby mediating stage-specific gene expression programs and post-meiotic chromatin reorganization. Genome-wide mapping data show that highly active Brdt-bound gene promoters systematically harbor competing histone acetylation and butyrylation marks at H4 K5 and H4 K8. Despite acting as a direct stimulator of transcription, histone butyrylation competes with acetylation, especially at H4 K5, to prevent Brdt binding. Additionally, H4 K5K8 butyrylation also marks retarded histone removal during late spermatogenesis. Hence, alternating H4 acetylation and butyrylation, while sustaining direct gene activation and dynamic bromodomain binding, could impact the final male epigenome features. Cell Press 2016-04-21 /pmc/articles/PMC4850424/ /pubmed/27105113 http://dx.doi.org/10.1016/j.molcel.2016.03.014 Text en © 2016 The Authors http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Article
Goudarzi, Afsaneh
Zhang, Di
Huang, He
Barral, Sophie
Kwon, Oh Kwang
Qi, Shankang
Tang, Zhanyun
Buchou, Thierry
Vitte, Anne-Laure
He, Tieming
Cheng, Zhongyi
Montellier, Emilie
Gaucher, Jonathan
Curtet, Sandrine
Debernardi, Alexandra
Charbonnier, Guillaume
Puthier, Denis
Petosa, Carlo
Panne, Daniel
Rousseaux, Sophie
Roeder, Robert G.
Zhao, Yingming
Khochbin, Saadi
Dynamic Competing Histone H4 K5K8 Acetylation and Butyrylation Are Hallmarks of Highly Active Gene Promoters
title Dynamic Competing Histone H4 K5K8 Acetylation and Butyrylation Are Hallmarks of Highly Active Gene Promoters
title_full Dynamic Competing Histone H4 K5K8 Acetylation and Butyrylation Are Hallmarks of Highly Active Gene Promoters
title_fullStr Dynamic Competing Histone H4 K5K8 Acetylation and Butyrylation Are Hallmarks of Highly Active Gene Promoters
title_full_unstemmed Dynamic Competing Histone H4 K5K8 Acetylation and Butyrylation Are Hallmarks of Highly Active Gene Promoters
title_short Dynamic Competing Histone H4 K5K8 Acetylation and Butyrylation Are Hallmarks of Highly Active Gene Promoters
title_sort dynamic competing histone h4 k5k8 acetylation and butyrylation are hallmarks of highly active gene promoters
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4850424/
https://www.ncbi.nlm.nih.gov/pubmed/27105113
http://dx.doi.org/10.1016/j.molcel.2016.03.014
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