Cancer-associated mutations of histones H2B, H3.1 and H2A.Z.1 affect the structure and stability of the nucleosome

Yasuhiro Arimura; Masae Ikura; Risa Fujita; Mamiko Noda; Wataru Kobayashi; Naoki Horikoshi; Jiying Sun; Lin Shi; Masayuki Kusakabe; Masahiko Harata; Yasuyuki Ohkawa; Satoshi Tashiro; Hiroshi Kimura; Tsuyoshi Ikura; Hitoshi Kurumizaka

doi:10.1093/nar/gky661

Cancer-associated mutations of histones H2B, H3.1 and H2A.Z.1 affect the structure and stability of the nucleosome

Yasuhiro Arimura, Masae Ikura, Risa Fujita, Mamiko Noda, Wataru Kobayashi, Naoki Horikoshi, Jiying Sun, Lin Shi, Masayuki Kusakabe, Masahiko Harata, Yasuyuki Ohkawa, Satoshi Tashiro, Hiroshi Kimura, Tsuyoshi Ikura, Hitoshi Kurumizaka

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Abstract

Mutations of the Glu76 residue of canonical histone H2B are frequently found in cancer cells. However, it is quite mysterious how a single amino acid substitution in one of the multiple H2B genes affects cell fate. Here we found that the H2B E76K mutation, in which Glu76 is replaced by Lys (E76K), distorted the interface between H2B and H4 in the nucleosome, as revealed by the crystal structure and induced nucleosome instability in vivo and in vitro. Exogenous production of the H2B E76Kmutant robustly enhanced the colony formation ability of the expressing cells, indicating that the H2B E76K mutant has the potential to promote oncogenic transformation in the presence of wild-type H2B. We found that other cancer-associated mutations of histones, H3.1 E97K and H2A.Z.1 R80C, also induced nucleosome instability. Interestingly, like the H2B E76K mutant, the H3.1 E97K mutant was minimally incorporated into chromatin in cells, but it enhanced the colony formation ability. In contrast, the H2A.Z.1 R80C mutant was incorporated into chromatin in cells, and had minor effects on the colony formation ability of the cells. These characteristics of histones with cancerassociated mutations may provide important information toward understanding how themutations promote cancer progression.

Original language	English
Pages (from-to)	10007-10018
Number of pages	12
Journal	Nucleic acids research
Volume	46
Issue number	19
DOIs	https://doi.org/10.1093/nar/gky661
Publication status	Published - 2018

All Science Journal Classification (ASJC) codes

Genetics

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1093/nar/gky661

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Arimura, Y., Ikura, M., Fujita, R., Noda, M., Kobayashi, W., Horikoshi, N., Sun, J., Shi, L., Kusakabe, M., Harata, M., Ohkawa, Y., Tashiro, S., Kimura, H., Ikura, T., & Kurumizaka, H. (2018). Cancer-associated mutations of histones H2B, H3.1 and H2A.Z.1 affect the structure and stability of the nucleosome. Nucleic acids research, 46(19), 10007-10018. https://doi.org/10.1093/nar/gky661

Arimura, Y, Ikura, M, Fujita, R, Noda, M, Kobayashi, W, Horikoshi, N, Sun, J, Shi, L, Kusakabe, M, Harata, M, Ohkawa, Y, Tashiro, S, Kimura, H, Ikura, T & Kurumizaka, H 2018, 'Cancer-associated mutations of histones H2B, H3.1 and H2A.Z.1 affect the structure and stability of the nucleosome', Nucleic acids research, vol. 46, no. 19, pp. 10007-10018. https://doi.org/10.1093/nar/gky661

@article{e9a8cece525347d6b823b9da6d8992a7,

title = "Cancer-associated mutations of histones H2B, H3.1 and H2A.Z.1 affect the structure and stability of the nucleosome",

abstract = "Mutations of the Glu76 residue of canonical histone H2B are frequently found in cancer cells. However, it is quite mysterious how a single amino acid substitution in one of the multiple H2B genes affects cell fate. Here we found that the H2B E76K mutation, in which Glu76 is replaced by Lys (E76K), distorted the interface between H2B and H4 in the nucleosome, as revealed by the crystal structure and induced nucleosome instability in vivo and in vitro. Exogenous production of the H2B E76Kmutant robustly enhanced the colony formation ability of the expressing cells, indicating that the H2B E76K mutant has the potential to promote oncogenic transformation in the presence of wild-type H2B. We found that other cancer-associated mutations of histones, H3.1 E97K and H2A.Z.1 R80C, also induced nucleosome instability. Interestingly, like the H2B E76K mutant, the H3.1 E97K mutant was minimally incorporated into chromatin in cells, but it enhanced the colony formation ability. In contrast, the H2A.Z.1 R80C mutant was incorporated into chromatin in cells, and had minor effects on the colony formation ability of the cells. These characteristics of histones with cancerassociated mutations may provide important information toward understanding how themutations promote cancer progression.",

author = "Yasuhiro Arimura and Masae Ikura and Risa Fujita and Mamiko Noda and Wataru Kobayashi and Naoki Horikoshi and Jiying Sun and Lin Shi and Masayuki Kusakabe and Masahiko Harata and Yasuyuki Ohkawa and Satoshi Tashiro and Hiroshi Kimura and Tsuyoshi Ikura and Hitoshi Kurumizaka",

note = "Funding Information: Waseda Research Institute for Science and Engineering; Research support programs of Waseda University; JSPS KAKENHI Grant [JP18H05534, JP25116002, JP17H01408 to H.Ku.; JP17K15043 to Y.A.; JP25116005 to H.Ki.; JP25116010 to Y.O.; JP16H01312 to S.T.; JP25116009 to M.H., JP16H01307 to T.I., in part]; JST CREST Grant [JPMJCR16G1 to H.Ku., H.Ki., Y.O., in part]; Platform Project for Supporting Drug Discovery and Life Science Research Japan Society for the Promotion of Science (Basis for Supporting Innovative Drug Discovery and Life Science Research (BINDS)) from AMED [JP18am0101076 to H.Ku., in part]; Uehara Memorial Foundation (to H.Ku.). Funding for open access charge: Waseda University. Conflict of interest statement. None declared. Publisher Copyright: {\textcopyright} The Author(s) 2018.",

year = "2018",

doi = "10.1093/nar/gky661",

language = "English",

volume = "46",

pages = "10007--10018",

journal = "Nucleic acids research",

issn = "0305-1048",

publisher = "Oxford University Press",

number = "19",

}

TY - JOUR

T1 - Cancer-associated mutations of histones H2B, H3.1 and H2A.Z.1 affect the structure and stability of the nucleosome

AU - Arimura, Yasuhiro

AU - Ikura, Masae

AU - Fujita, Risa

AU - Noda, Mamiko

AU - Kobayashi, Wataru

AU - Horikoshi, Naoki

AU - Sun, Jiying

AU - Shi, Lin

AU - Kusakabe, Masayuki

AU - Harata, Masahiko

AU - Ohkawa, Yasuyuki

AU - Tashiro, Satoshi

AU - Kimura, Hiroshi

AU - Ikura, Tsuyoshi

AU - Kurumizaka, Hitoshi

N1 - Funding Information: Waseda Research Institute for Science and Engineering; Research support programs of Waseda University; JSPS KAKENHI Grant [JP18H05534, JP25116002, JP17H01408 to H.Ku.; JP17K15043 to Y.A.; JP25116005 to H.Ki.; JP25116010 to Y.O.; JP16H01312 to S.T.; JP25116009 to M.H., JP16H01307 to T.I., in part]; JST CREST Grant [JPMJCR16G1 to H.Ku., H.Ki., Y.O., in part]; Platform Project for Supporting Drug Discovery and Life Science Research Japan Society for the Promotion of Science (Basis for Supporting Innovative Drug Discovery and Life Science Research (BINDS)) from AMED [JP18am0101076 to H.Ku., in part]; Uehara Memorial Foundation (to H.Ku.). Funding for open access charge: Waseda University. Conflict of interest statement. None declared. Publisher Copyright: © The Author(s) 2018.

PY - 2018

Y1 - 2018

N2 - Mutations of the Glu76 residue of canonical histone H2B are frequently found in cancer cells. However, it is quite mysterious how a single amino acid substitution in one of the multiple H2B genes affects cell fate. Here we found that the H2B E76K mutation, in which Glu76 is replaced by Lys (E76K), distorted the interface between H2B and H4 in the nucleosome, as revealed by the crystal structure and induced nucleosome instability in vivo and in vitro. Exogenous production of the H2B E76Kmutant robustly enhanced the colony formation ability of the expressing cells, indicating that the H2B E76K mutant has the potential to promote oncogenic transformation in the presence of wild-type H2B. We found that other cancer-associated mutations of histones, H3.1 E97K and H2A.Z.1 R80C, also induced nucleosome instability. Interestingly, like the H2B E76K mutant, the H3.1 E97K mutant was minimally incorporated into chromatin in cells, but it enhanced the colony formation ability. In contrast, the H2A.Z.1 R80C mutant was incorporated into chromatin in cells, and had minor effects on the colony formation ability of the cells. These characteristics of histones with cancerassociated mutations may provide important information toward understanding how themutations promote cancer progression.

AB - Mutations of the Glu76 residue of canonical histone H2B are frequently found in cancer cells. However, it is quite mysterious how a single amino acid substitution in one of the multiple H2B genes affects cell fate. Here we found that the H2B E76K mutation, in which Glu76 is replaced by Lys (E76K), distorted the interface between H2B and H4 in the nucleosome, as revealed by the crystal structure and induced nucleosome instability in vivo and in vitro. Exogenous production of the H2B E76Kmutant robustly enhanced the colony formation ability of the expressing cells, indicating that the H2B E76K mutant has the potential to promote oncogenic transformation in the presence of wild-type H2B. We found that other cancer-associated mutations of histones, H3.1 E97K and H2A.Z.1 R80C, also induced nucleosome instability. Interestingly, like the H2B E76K mutant, the H3.1 E97K mutant was minimally incorporated into chromatin in cells, but it enhanced the colony formation ability. In contrast, the H2A.Z.1 R80C mutant was incorporated into chromatin in cells, and had minor effects on the colony formation ability of the cells. These characteristics of histones with cancerassociated mutations may provide important information toward understanding how themutations promote cancer progression.

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U2 - 10.1093/nar/gky661

DO - 10.1093/nar/gky661

M3 - Article

C2 - 30053102

AN - SCOPUS:85056260677

SN - 0305-1048

VL - 46

SP - 10007

EP - 10018

JO - Nucleic acids research

JF - Nucleic acids research

IS - 19

ER -

Cancer-associated mutations of histones H2B, H3.1 and H2A.Z.1 affect the structure and stability of the nucleosome

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