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  1. 原著論文

Designer Catalyst-Enabled Regiodivergent Histone Acetylation

https://repo.qst.go.jp/records/2001212
https://repo.qst.go.jp/records/2001212
8f6bad48-0e14-47d5-a88e-0f232a3ca0af
アイテムタイプ 学術雑誌論文 / Journal Article(1)
公開日 2025-08-05
タイトル
タイトル Designer Catalyst-Enabled Regiodivergent Histone Acetylation
言語 en
言語
言語 eng
資源タイプ
資源タイプ識別子 http://purl.org/coar/resource_type/c_6501
資源タイプ journal article
著者 Tamiko Nozaki

× Tamiko Nozaki

Tamiko Nozaki

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Mayu Onoda

× Mayu Onoda

Mayu Onoda

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Misuzu Habazaki

× Misuzu Habazaki

Misuzu Habazaki

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Yuma Takeuchi

× Yuma Takeuchi

Yuma Takeuchi

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Ishida Hisashi

× Ishida Hisashi

Ishida Hisashi

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Yuko Sato

× Yuko Sato

Yuko Sato

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Tomoya Kujirai

× Tomoya Kujirai

Tomoya Kujirai

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Kayo Hanada

× Kayo Hanada

Kayo Hanada

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Kenzo Yamatsugu

× Kenzo Yamatsugu

Kenzo Yamatsugu

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Hitoshi Kurumizaka

× Hitoshi Kurumizaka

Hitoshi Kurumizaka

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Hiroshi Kimura

× Hiroshi Kimura

Hiroshi Kimura

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Kono Hidetoshi

× Kono Hidetoshi

Kono Hidetoshi

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Shigehiro A. Kawashima

× Shigehiro A. Kawashima

Shigehiro A. Kawashima

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Motomu Kanai

× Motomu Kanai

Motomu Kanai

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抄録
内容記述タイプ Abstract
内容記述 The “histone code,” defined by the combinatorial patterns of post-translational modifications (PTMs) on histones, plays a pivotal role in chromatin structure and gene expression. Tools for the regioselective introduction of histone PTMs in living cells are critical for dissecting the functions of these epigenetic marks. Here, we report the design and development of three regioselective catalysts that acetylate distinct lysine residues (K43, K108, and K120) on histone H2B. Using a combination of molecular dynamics simulations of catalyst-nucleosome complexes and systematic experimental optimization of catalyst structures, we identified key design principles for achieving regioselectivity. Specifically, excluding highly reactive off-target lysine residues from the catalyst effective region (CER) while maintaining proximity to a target lysine residue proved crucial. Biochemical and cellular analyses of the catalytic histone acetylation revealed that each lysine acetylation elicited unique effects on the binding affinity and activity of nucleosome-interacting molecules, as well as on transcriptional programs and cellular phenotypes. These findings establish a framework for designing regioselective histone acetylation catalysts and advance our understanding of the regulatory mechanisms underlying histone PTMs.
書誌情報 Journal of the American Chemical Society

巻 147, 号 16, p. 13732-13743, 発行日 2025-04
出版者
出版者 アメリカ化学会
DOI
識別子タイプ DOI
関連識別子 10.1021/jacs.5c01699
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