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Phosphorylation of histone H3T6 by PKCβ_I controls demethylation at histone H3K4

The amino-terminal tails of histone proteins are subject to a variety of post-translational modifications; addition or removal of these 'marks' facilitates gene activation or silencing. Here, a mechanism is defined that modulates the activity of the dual-specificity histone demethylase LSD1 during androgen-dependent transcription. Androgen-dependent signalling through protein kinase C beta I leads to phosphorylation of a histone amino acid, which prevents demethylation of an adjacent amino acid by LSD1.

Eric Metzger
Axel Imhof
Roland Schüle
Research14 Mar 2010
Nature

Volume: 464, P: 792-796
Mitochondrial KMT9 methylates DLAT to control pyruvate dehydrogenase activity and prostate cancer growth

Prostate cancer growth depends on de novo lipogenesis controlled by the mitochondrial pyruvate dehydrogenase complex (PDC). Here the authors find that a histone methyltransferase KMT9 is localized in the mitochondria of prostate cancer cells to regulate PDC activity by methylating its subunit DLAT.

Yanhan Jia
Sheng Wang
Roland Schüle
ResearchOpen Access30 Jan 2025
Nature Communications

Volume: 16, P: 1-14
Cooperative demethylation by JMJD2C and LSD1 promotes androgen receptor-dependent gene expression

Melanie Wissmann
Na Yin
Roland Schüle
Research04 Feb 2007
Nature Cell Biology

Volume: 9, P: 347-353
Structure-guided design of a selective inhibitor of the methyltransferase KMT9 with cellular activity

Wang et al. report on an inhibitor of the lysine methyltransferase KMT9 with cellular activity. The inhibitor blocks proliferation of androgen-resistant prostate cancer cells, opening therapeutics avenues to treat this type of cancer.

Sheng Wang
Sebastian O. Klein
Roland Schüle
ResearchOpen Access02 Jan 2024
Nature Communications

Volume: 15, P: 1-12
KMT9 monomethylates histone H4 lysine 12 and controls proliferation of prostate cancer cells

KMT9, a new histone lysine methyltransferase targeting H4K12, is enriched at promoters of genes encoding molecules involved in the cell cycle and controls the growth of androgen receptor–dependent and castration- and enzalutamide-resistant prostate cancer cells and xenograft tumors.

Eric Metzger
Sheng Wang
Roland Schüle
Research06 May 2019
Nature Structural & Molecular Biology

Volume: 26, P: 361-371
LSD1 promotes oxidative metabolism of white adipose tissue

Brown adipocytes are rich in mitochondria and influence whole-body energy balance. Here, Duteil et al. show that the lysine-specific demethylase 1 (LSD1) controls mitochondrial biogenesis and the formation of brown-like adipocytes, and that LSD1 overexpression in white fat reduces weight gain of mice on a high-fat diet.

Delphine Duteil
Eric Metzger
Roland Schüle
Research10 Jun 2014
Nature Communications

Volume: 5, P: 1-14
The histone code reader Spin1 controls skeletal muscle development

Holger Greschik
Delphine Duteil
Roland Schüle
ResearchOpen Access23 Nov 2017
Cell Death & Disease

Volume: 8, P: e3173

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Phosphorylation of histone H3T6 by PKCβI controls demethylation at histone H3K4

Mitochondrial KMT9 methylates DLAT to control pyruvate dehydrogenase activity and prostate cancer growth

Cooperative demethylation by JMJD2C and LSD1 promotes androgen receptor-dependent gene expression

Structure-guided design of a selective inhibitor of the methyltransferase KMT9 with cellular activity

KMT9 monomethylates histone H4 lysine 12 and controls proliferation of prostate cancer cells

LSD1 promotes oxidative metabolism of white adipose tissue

The histone code reader Spin1 controls skeletal muscle development

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Phosphorylation of histone H3T6 by PKCβ_I controls demethylation at histone H3K4