Chd5 orchestrates chromatin remodelling during sperm development

Wangzhi Li; Jie Wu; Sang Yong Kim; Ming Zhao; Stephen A. Hearn; Michael Q. Zhang; Marvin L. Meistrich; Alea A. Mills

doi:10.1038/ncomms4812

Chd5 orchestrates chromatin remodelling during sperm development

Wangzhi Li, Jie Wu, Sang Yong Kim, Ming Zhao, Stephen A. Hearn, Michael Q. Zhang, Marvin L. Meistrich, Alea A. Mills

School of Health Professions

Research output: Contribution to journal › Article › peer-review

76 Scopus citations

Abstract

One of the most remarkable chromatin remodelling processes occurs during spermiogenesis, the post-meiotic phase of sperm development during which histones are replaced with sperm-specific protamines to repackage the genome into the highly compact chromatin structure of mature sperm. Here we identify Chromodomain helicase DNA binding protein 5 (Chd5) as a master regulator of the histone-to-protamine chromatin remodelling process. Chd5 deficiency leads to defective sperm chromatin compaction and male infertility in mice, mirroring the observation of low CHD5 expression in testes of infertile men. Chd5 orchestrates a cascade of molecular events required for histone removal and replacement, including histone 4 (H4) hyperacetylation, histone variant expression, nucleosome eviction and DNA damage repair. Chd5 deficiency also perturbs expression of transition proteins (Tnp1/Tnp2) and protamines (Prm1/2). These findings define Chd5 as a multi-faceted mediator of histone-to-protamine replacement and depict the cascade of molecular events underlying this process of extensive chromatin remodelling.

Original language	English (US)
Article number	3812
Journal	Nature communications
Volume	5
DOIs	https://doi.org/10.1038/ncomms4812
State	Published - May 13 2014

ASJC Scopus subject areas

General Chemistry
General Biochemistry, Genetics and Molecular Biology
General Physics and Astronomy

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title = "Chd5 orchestrates chromatin remodelling during sperm development",

abstract = "One of the most remarkable chromatin remodelling processes occurs during spermiogenesis, the post-meiotic phase of sperm development during which histones are replaced with sperm-specific protamines to repackage the genome into the highly compact chromatin structure of mature sperm. Here we identify Chromodomain helicase DNA binding protein 5 (Chd5) as a master regulator of the histone-to-protamine chromatin remodelling process. Chd5 deficiency leads to defective sperm chromatin compaction and male infertility in mice, mirroring the observation of low CHD5 expression in testes of infertile men. Chd5 orchestrates a cascade of molecular events required for histone removal and replacement, including histone 4 (H4) hyperacetylation, histone variant expression, nucleosome eviction and DNA damage repair. Chd5 deficiency also perturbs expression of transition proteins (Tnp1/Tnp2) and protamines (Prm1/2). These findings define Chd5 as a multi-faceted mediator of histone-to-protamine replacement and depict the cascade of molecular events underlying this process of extensive chromatin remodelling.",

author = "Wangzhi Li and Jie Wu and Kim, {Sang Yong} and Ming Zhao and Hearn, {Stephen A.} and Zhang, {Michael Q.} and Meistrich, {Marvin L.} and Mills, {Alea A.}",

note = "Funding Information: We thank W. Stephen Kistler for anti-Tnp antibodies, Jo H.M. Berden for anti-nucleosome antibodies, Emma Vernersson-Lindahl for critical reading of the manuscript, and Lisa Bianco and Aigoul Nourjanova for technical assistance. This project was supported by the Office of the Director, National Institutes of Health under award numbers R01CA127383 (to A.A.M.) and R21OD018332 (to A.A.M.), NIH HG001696 (to M.Q.Z.), and NSFC 91019016 (to M.Q.Z.); the content is the sole responsibility of the authors. This work was performed with assistance from Cold Spring Harbour Laboratory Shared Resources, which are funded, in part, by the Cancer Center Support Grant 5P30CA045508.",

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AU - Meistrich, Marvin L.

AU - Mills, Alea A.

N1 - Funding Information: We thank W. Stephen Kistler for anti-Tnp antibodies, Jo H.M. Berden for anti-nucleosome antibodies, Emma Vernersson-Lindahl for critical reading of the manuscript, and Lisa Bianco and Aigoul Nourjanova for technical assistance. This project was supported by the Office of the Director, National Institutes of Health under award numbers R01CA127383 (to A.A.M.) and R21OD018332 (to A.A.M.), NIH HG001696 (to M.Q.Z.), and NSFC 91019016 (to M.Q.Z.); the content is the sole responsibility of the authors. This work was performed with assistance from Cold Spring Harbour Laboratory Shared Resources, which are funded, in part, by the Cancer Center Support Grant 5P30CA045508.

PY - 2014/5/13

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N2 - One of the most remarkable chromatin remodelling processes occurs during spermiogenesis, the post-meiotic phase of sperm development during which histones are replaced with sperm-specific protamines to repackage the genome into the highly compact chromatin structure of mature sperm. Here we identify Chromodomain helicase DNA binding protein 5 (Chd5) as a master regulator of the histone-to-protamine chromatin remodelling process. Chd5 deficiency leads to defective sperm chromatin compaction and male infertility in mice, mirroring the observation of low CHD5 expression in testes of infertile men. Chd5 orchestrates a cascade of molecular events required for histone removal and replacement, including histone 4 (H4) hyperacetylation, histone variant expression, nucleosome eviction and DNA damage repair. Chd5 deficiency also perturbs expression of transition proteins (Tnp1/Tnp2) and protamines (Prm1/2). These findings define Chd5 as a multi-faceted mediator of histone-to-protamine replacement and depict the cascade of molecular events underlying this process of extensive chromatin remodelling.

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Chd5 orchestrates chromatin remodelling during sperm development

Abstract

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