Reader domain specificity and lysine demethylase-4 family function

Zhangli Su; Fengbin Wang; Jin Hee Lee; Kimberly E. Stephens; Romeo Papazyan; Ekaterina Voronina; Kimberly A. Krautkramer; Ana Raman; Jeremy J. Thorpe; Melissa D. Boersma; Vyacheslav I. Kuznetsov; Mitchell D. Miller; Sean D. Taverna; George N. Phillips; John M. Denu

doi:10.1038/ncomms13387

Reader domain specificity and lysine demethylase-4 family function

Zhangli Su, Fengbin Wang, Jin Hee Lee, Kimberly E. Stephens, Romeo Papazyan, Ekaterina Voronina, Kimberly A. Krautkramer, Ana Raman, Jeremy J. Thorpe, Melissa D. Boersma, Vyacheslav I. Kuznetsov, Mitchell D. Miller, Sean D. Taverna, George N. Phillips, John M. Denu

School of Medicine

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

22 Scopus citations

Abstract

The KDM4 histone demethylases are conserved epigenetic regulators linked to development, spermatogenesis and tumorigenesis. However, how the KDM4 family targets specific chromatin regions is largely unknown. Here, an extensive histone peptide microarray analysis uncovers trimethyl-lysine histone-binding preferences among the closely related KDM4 double tudor domains (DTDs). KDM4A/B DTDs bind strongly to H3K23me3, a poorly understood histone modification recently shown to be enriched in meiotic chromatin of ciliates and nematodes. The 2.28 Å co-crystal structure of KDM4A-DTD in complex with H3K23me3 peptide reveals key intermolecular interactions for H3K23me3 recognition. Furthermore, analysis of the 2.56 Å KDM4B-DTD crystal structure pinpoints the underlying residues required for exclusive H3K23me3 specificity, an interaction supported by in vivo co-localization of KDM4B and H3K23me3 at heterochromatin in mammalian meiotic and newly postmeiotic spermatocytes. In vitro demethylation assays suggest H3K23me3 binding by KDM4B stimulates H3K36 demethylation. Together, these results provide a possible mechanism whereby H3K23me3-binding by KDM4B directs localized H3K36 demethylation during meiosis and spermatogenesis.

Original language	English (US)
Article number	13387
Journal	Nature communications
Volume	7
DOIs	https://doi.org/10.1038/ncomms13387
State	Published - Nov 14 2016

ASJC Scopus subject areas

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

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10.1038/ncomms13387

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title = "Reader domain specificity and lysine demethylase-4 family function",

abstract = "The KDM4 histone demethylases are conserved epigenetic regulators linked to development, spermatogenesis and tumorigenesis. However, how the KDM4 family targets specific chromatin regions is largely unknown. Here, an extensive histone peptide microarray analysis uncovers trimethyl-lysine histone-binding preferences among the closely related KDM4 double tudor domains (DTDs). KDM4A/B DTDs bind strongly to H3K23me3, a poorly understood histone modification recently shown to be enriched in meiotic chromatin of ciliates and nematodes. The 2.28 {\AA} co-crystal structure of KDM4A-DTD in complex with H3K23me3 peptide reveals key intermolecular interactions for H3K23me3 recognition. Furthermore, analysis of the 2.56 {\AA} KDM4B-DTD crystal structure pinpoints the underlying residues required for exclusive H3K23me3 specificity, an interaction supported by in vivo co-localization of KDM4B and H3K23me3 at heterochromatin in mammalian meiotic and newly postmeiotic spermatocytes. In vitro demethylation assays suggest H3K23me3 binding by KDM4B stimulates H3K36 demethylation. Together, these results provide a possible mechanism whereby H3K23me3-binding by KDM4B directs localized H3K36 demethylation during meiosis and spermatogenesis.",

author = "Zhangli Su and Fengbin Wang and Lee, {Jin Hee} and Stephens, {Kimberly E.} and Romeo Papazyan and Ekaterina Voronina and Krautkramer, {Kimberly A.} and Ana Raman and Thorpe, {Jeremy J.} and Boersma, {Melissa D.} and Kuznetsov, {Vyacheslav I.} and Miller, {Mitchell D.} and Taverna, {Sean D.} and Phillips, {George N.} and Denu, {John M.}",

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AU - Su, Zhangli

AU - Wang, Fengbin

AU - Lee, Jin Hee

AU - Stephens, Kimberly E.

AU - Papazyan, Romeo

AU - Voronina, Ekaterina

AU - Krautkramer, Kimberly A.

AU - Raman, Ana

AU - Thorpe, Jeremy J.

AU - Boersma, Melissa D.

AU - Kuznetsov, Vyacheslav I.

AU - Miller, Mitchell D.

AU - Taverna, Sean D.

AU - Phillips, George N.

AU - Denu, John M.

PY - 2016/11/14

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AB - The KDM4 histone demethylases are conserved epigenetic regulators linked to development, spermatogenesis and tumorigenesis. However, how the KDM4 family targets specific chromatin regions is largely unknown. Here, an extensive histone peptide microarray analysis uncovers trimethyl-lysine histone-binding preferences among the closely related KDM4 double tudor domains (DTDs). KDM4A/B DTDs bind strongly to H3K23me3, a poorly understood histone modification recently shown to be enriched in meiotic chromatin of ciliates and nematodes. The 2.28 Å co-crystal structure of KDM4A-DTD in complex with H3K23me3 peptide reveals key intermolecular interactions for H3K23me3 recognition. Furthermore, analysis of the 2.56 Å KDM4B-DTD crystal structure pinpoints the underlying residues required for exclusive H3K23me3 specificity, an interaction supported by in vivo co-localization of KDM4B and H3K23me3 at heterochromatin in mammalian meiotic and newly postmeiotic spermatocytes. In vitro demethylation assays suggest H3K23me3 binding by KDM4B stimulates H3K36 demethylation. Together, these results provide a possible mechanism whereby H3K23me3-binding by KDM4B directs localized H3K36 demethylation during meiosis and spermatogenesis.

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Reader domain specificity and lysine demethylase-4 family function

Abstract

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