Sumo modification system facilitates the exchange of histone variant h2a.Z-2 at dna damage sites

Atsuhiko Fukuto; Masae Ikura; Tsuyoshi Ikura; Jiying Sun; Yasunori Horikoshi; Hiroki Shima; Kazuhiko Igarashi; Masayuki Kusakabe; Masahiko Harata; Naoki Horikoshi; Hitoshi Kurumizaka; Yoshiaki Kiuchi; Satoshi Tashiro

doi:10.1080/19491034.2017.1395543

Sumo modification system facilitates the exchange of histone variant h2a.Z-2 at dna damage sites

Atsuhiko Fukuto, Masae Ikura, Tsuyoshi Ikura, Jiying Sun, Yasunori Horikoshi, Hiroki Shima, Kazuhiko Igarashi, Masayuki Kusakabe, Masahiko Harata, Naoki Horikoshi, Hitoshi Kurumizaka, Yoshiaki Kiuchi, Satoshi Tashiro

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

16 Citations (Scopus)

Abstract

Histone exchange and histone post-translational modifications play important roles in the regulation of DNA metabolism, by re-organizing the chromatin configuration. We previously demonstrated that the histone variant H2A.Z-2 is rapidly exchanged at damaged sites after DNA double strand break induction in human cells. In yeast, the small ubiquitin-like modifier (SUMO) modification of H2A.Z is involved in the DNA damage response. However, whether the SUMO modification regulates the exchange of human H2A.Z-2 at DNA damage sites remains unclear. Here, we show that H2A.Z-2 is SUMOylated in a damage-dependent manner, and the SUMOylation of H2A.Z-2 is suppressed by the depletion of the SUMO E3 ligase, PIAS4. Moreover, PIAS4 depletion represses the incorporation and eviction of H2A.Z-2 at damaged sites. These findings demonstrate that the PIAS4-mediated SUMOylation regulates the exchange of H2A.Z-2 at DNA damage sites.

Original language	English
Pages (from-to)	87-94
Number of pages	8
Journal	Nucleus
Volume	9
Issue number	1
DOIs	https://doi.org/10.1080/19491034.2017.1395543
Publication status	Published - 2018 Dec 12

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title = "Sumo modification system facilitates the exchange of histone variant h2a.Z-2 at dna damage sites",

abstract = "Histone exchange and histone post-translational modifications play important roles in the regulation of DNA metabolism, by re-organizing the chromatin configuration. We previously demonstrated that the histone variant H2A.Z-2 is rapidly exchanged at damaged sites after DNA double strand break induction in human cells. In yeast, the small ubiquitin-like modifier (SUMO) modification of H2A.Z is involved in the DNA damage response. However, whether the SUMO modification regulates the exchange of human H2A.Z-2 at DNA damage sites remains unclear. Here, we show that H2A.Z-2 is SUMOylated in a damage-dependent manner, and the SUMOylation of H2A.Z-2 is suppressed by the depletion of the SUMO E3 ligase, PIAS4. Moreover, PIAS4 depletion represses the incorporation and eviction of H2A.Z-2 at damaged sites. These findings demonstrate that the PIAS4-mediated SUMOylation regulates the exchange of H2A.Z-2 at DNA damage sites.",

author = "Atsuhiko Fukuto and Masae Ikura and Tsuyoshi Ikura and Jiying Sun and Yasunori Horikoshi and Hiroki Shima and Kazuhiko Igarashi and Masayuki Kusakabe and Masahiko Harata and Naoki Horikoshi and Hitoshi Kurumizaka and Yoshiaki Kiuchi and Satoshi Tashiro",

note = "Funding Information: This research was supported by JSPS KAKENHI Grants, number JP26430114 to J.S., number JP25116009 to M.H. and numbers JP16H01312 and JP15H02821 to S.T. This work was partially supported by the Program of the network-type joint Usage/Research Center for Radiation Disaster Medical Science of Hiroshima University, Nagasaki University, and Fukushima Medical University Publisher Copyright: {\textcopyright} 2018, The authors.",

year = "2018",

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doi = "10.1080/19491034.2017.1395543",

language = "English",

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AU - Fukuto, Atsuhiko

AU - Ikura, Masae

AU - Ikura, Tsuyoshi

AU - Sun, Jiying

AU - Horikoshi, Yasunori

AU - Shima, Hiroki

AU - Igarashi, Kazuhiko

AU - Kusakabe, Masayuki

AU - Harata, Masahiko

AU - Horikoshi, Naoki

AU - Kurumizaka, Hitoshi

AU - Kiuchi, Yoshiaki

AU - Tashiro, Satoshi

N1 - Funding Information: This research was supported by JSPS KAKENHI Grants, number JP26430114 to J.S., number JP25116009 to M.H. and numbers JP16H01312 and JP15H02821 to S.T. This work was partially supported by the Program of the network-type joint Usage/Research Center for Radiation Disaster Medical Science of Hiroshima University, Nagasaki University, and Fukushima Medical University Publisher Copyright: © 2018, The authors.

PY - 2018/12/12

Y1 - 2018/12/12

N2 - Histone exchange and histone post-translational modifications play important roles in the regulation of DNA metabolism, by re-organizing the chromatin configuration. We previously demonstrated that the histone variant H2A.Z-2 is rapidly exchanged at damaged sites after DNA double strand break induction in human cells. In yeast, the small ubiquitin-like modifier (SUMO) modification of H2A.Z is involved in the DNA damage response. However, whether the SUMO modification regulates the exchange of human H2A.Z-2 at DNA damage sites remains unclear. Here, we show that H2A.Z-2 is SUMOylated in a damage-dependent manner, and the SUMOylation of H2A.Z-2 is suppressed by the depletion of the SUMO E3 ligase, PIAS4. Moreover, PIAS4 depletion represses the incorporation and eviction of H2A.Z-2 at damaged sites. These findings demonstrate that the PIAS4-mediated SUMOylation regulates the exchange of H2A.Z-2 at DNA damage sites.

AB - Histone exchange and histone post-translational modifications play important roles in the regulation of DNA metabolism, by re-organizing the chromatin configuration. We previously demonstrated that the histone variant H2A.Z-2 is rapidly exchanged at damaged sites after DNA double strand break induction in human cells. In yeast, the small ubiquitin-like modifier (SUMO) modification of H2A.Z is involved in the DNA damage response. However, whether the SUMO modification regulates the exchange of human H2A.Z-2 at DNA damage sites remains unclear. Here, we show that H2A.Z-2 is SUMOylated in a damage-dependent manner, and the SUMOylation of H2A.Z-2 is suppressed by the depletion of the SUMO E3 ligase, PIAS4. Moreover, PIAS4 depletion represses the incorporation and eviction of H2A.Z-2 at damaged sites. These findings demonstrate that the PIAS4-mediated SUMOylation regulates the exchange of H2A.Z-2 at DNA damage sites.

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Sumo modification system facilitates the exchange of histone variant h2a.Z-2 at dna damage sites

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