Cryo-EM structure of the nucleosome core particle containing Giardia lamblia histones

Shoko Sato; Yoshimasa Takizawa; Fumika Hoshikawa; Mariko Dacher; Hiroki Tanaka; Hiroaki Tachiwana; Tomoya Kujirai; Yukari Iikura; Cheng Han Ho; Naruhiko Adachi; Indu Patwal; Andrew Flaus; Hitoshi Kurumizaka

doi:10.1093/nar/gkab644

Cryo-EM structure of the nucleosome core particle containing Giardia lamblia histones

Shoko Sato
, Yoshimasa Takizawa
, Fumika Hoshikawa
, Mariko Dacher
, Hiroki Tanaka
, Hiroaki Tachiwana
, Tomoya Kujirai
, Yukari Iikura
, Cheng Han Ho
, Naruhiko Adachi
, Indu Patwal
, Andrew Flaus
, Hitoshi Kurumizaka

Molecular Biosciences

Research output: Contribution to a Journal (Peer & Non Peer) › Article › peer-review

17 Citations (Scopus)

Abstract

Giardia lamblia is a pathogenic unicellular eukaryotic parasite that causes giardiasis. Its genome encodes the canonical histones H2A, H2B, H3, and H4, which share low amino acid sequence identity with their human orthologues. We determined the structure of the G. lamblia nucleosome core particle (NCP) at 3.6 Å resolution by cryo-electron microscopy. G. lamblia histones form a characteristic NCP, in which the visible 125 base-pair region of the DNA is wrapped in a left-handed supercoil. The acidic patch on the G. lamblia octamer is deeper, due to an insertion extending the H2B α1 helix and L1 loop, and thus cannot bind the LANA acidic patch binding peptide. The DNA and histone regions near the DNA entry-exit sites could not be assigned, suggesting that these regions are asymmetrically flexible in the G. lamblia NCP. Characterization by thermal unfolding in solution revealed that both the H2A-H2B and DNA association with the G. lamblia H3-H4 were weaker than those for human H3-H4. These results demonstrate the uniformity of the histone octamer as the organizing platform for eukaryotic chromatin, but also illustrate the unrecognized capability for large scale sequence variations that enable the adaptability of histone octamer surfaces and confer internal stability.

Original language	English
Pages (from-to)	8934-8946
Number of pages	13
Journal	Nucleic Acids Research
Volume	49
Issue number	15
DOIs	https://doi.org/10.1093/nar/gkab644
Publication status	Published - 7 Sep 2021

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title = "Cryo-EM structure of the nucleosome core particle containing Giardia lamblia histones",

abstract = "Giardia lamblia is a pathogenic unicellular eukaryotic parasite that causes giardiasis. Its genome encodes the canonical histones H2A, H2B, H3, and H4, which share low amino acid sequence identity with their human orthologues. We determined the structure of the G. lamblia nucleosome core particle (NCP) at 3.6 {\AA} resolution by cryo-electron microscopy. G. lamblia histones form a characteristic NCP, in which the visible 125 base-pair region of the DNA is wrapped in a left-handed supercoil. The acidic patch on the G. lamblia octamer is deeper, due to an insertion extending the H2B α1 helix and L1 loop, and thus cannot bind the LANA acidic patch binding peptide. The DNA and histone regions near the DNA entry-exit sites could not be assigned, suggesting that these regions are asymmetrically flexible in the G. lamblia NCP. Characterization by thermal unfolding in solution revealed that both the H2A-H2B and DNA association with the G. lamblia H3-H4 were weaker than those for human H3-H4. These results demonstrate the uniformity of the histone octamer as the organizing platform for eukaryotic chromatin, but also illustrate the unrecognized capability for large scale sequence variations that enable the adaptability of histone octamer surfaces and confer internal stability.",

author = "Shoko Sato and Yoshimasa Takizawa and Fumika Hoshikawa and Mariko Dacher and Hiroki Tanaka and Hiroaki Tachiwana and Tomoya Kujirai and Yukari Iikura and Ho, \{Cheng Han\} and Naruhiko Adachi and Indu Patwal and Andrew Flaus and Hitoshi Kurumizaka",

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AU - Sato, Shoko

AU - Takizawa, Yoshimasa

AU - Hoshikawa, Fumika

AU - Dacher, Mariko

AU - Tanaka, Hiroki

AU - Tachiwana, Hiroaki

AU - Kujirai, Tomoya

AU - Iikura, Yukari

AU - Ho, Cheng Han

AU - Adachi, Naruhiko

AU - Patwal, Indu

AU - Flaus, Andrew

AU - Kurumizaka, Hitoshi

PY - 2021/9/7

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N2 - Giardia lamblia is a pathogenic unicellular eukaryotic parasite that causes giardiasis. Its genome encodes the canonical histones H2A, H2B, H3, and H4, which share low amino acid sequence identity with their human orthologues. We determined the structure of the G. lamblia nucleosome core particle (NCP) at 3.6 Å resolution by cryo-electron microscopy. G. lamblia histones form a characteristic NCP, in which the visible 125 base-pair region of the DNA is wrapped in a left-handed supercoil. The acidic patch on the G. lamblia octamer is deeper, due to an insertion extending the H2B α1 helix and L1 loop, and thus cannot bind the LANA acidic patch binding peptide. The DNA and histone regions near the DNA entry-exit sites could not be assigned, suggesting that these regions are asymmetrically flexible in the G. lamblia NCP. Characterization by thermal unfolding in solution revealed that both the H2A-H2B and DNA association with the G. lamblia H3-H4 were weaker than those for human H3-H4. These results demonstrate the uniformity of the histone octamer as the organizing platform for eukaryotic chromatin, but also illustrate the unrecognized capability for large scale sequence variations that enable the adaptability of histone octamer surfaces and confer internal stability.

AB - Giardia lamblia is a pathogenic unicellular eukaryotic parasite that causes giardiasis. Its genome encodes the canonical histones H2A, H2B, H3, and H4, which share low amino acid sequence identity with their human orthologues. We determined the structure of the G. lamblia nucleosome core particle (NCP) at 3.6 Å resolution by cryo-electron microscopy. G. lamblia histones form a characteristic NCP, in which the visible 125 base-pair region of the DNA is wrapped in a left-handed supercoil. The acidic patch on the G. lamblia octamer is deeper, due to an insertion extending the H2B α1 helix and L1 loop, and thus cannot bind the LANA acidic patch binding peptide. The DNA and histone regions near the DNA entry-exit sites could not be assigned, suggesting that these regions are asymmetrically flexible in the G. lamblia NCP. Characterization by thermal unfolding in solution revealed that both the H2A-H2B and DNA association with the G. lamblia H3-H4 were weaker than those for human H3-H4. These results demonstrate the uniformity of the histone octamer as the organizing platform for eukaryotic chromatin, but also illustrate the unrecognized capability for large scale sequence variations that enable the adaptability of histone octamer surfaces and confer internal stability.

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U2 - 10.1093/nar/gkab644

DO - 10.1093/nar/gkab644

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EP - 8946

JO - Nucleic Acids Research

JF - Nucleic Acids Research

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ER -

Cryo-EM structure of the nucleosome core particle containing Giardia lamblia histones

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