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A Tail-Based Mechanism Drives Nucleosome Demethylation by the LSD2/NPAC Multimeric Complex

Academic Article
Publication Date:
2019
abstract:
LSD1 and LSD2 are homologous histone demethylases with opposite biological outcomes related to chromatin silencing and transcription elongation, respectively. Unlike LSD1, LSD2 nucleosome-demethylase activity relies on a specific linker peptide from the multidomain protein NPAC. We used single-particle cryoelectron microscopy (cryo-EM), in combination with kinetic and mutational analysis, to analyze the mechanisms underlying the function of the human LSD2/NPAC-linker/ nucleosome complex. Weak interactions between LSD2 and DNA enable multiple binding modes for the association of the demethylase to the nucleosome. The demethylase thereby captures mono-and dimethyl Lys4 of the H3 tail to afford histone demethylation. Our studies also establish that the dehydrogenase domain of NPAC serves as a catalytically inert oligomerization module. While LSD1/CoREST forms a nucleosome docking platform at silenced gene promoters, LSD2/NPAC is a multifunctional enzyme complex with flexible linkers, tailored for rapid chromatin modification, in conjunction with the advance of the RNA polymerase on actively transcribed genes.
Iris type:
1.1 Articolo in rivista
Keywords:
chromatin reader; cryoelectron microscopy; epigenetics; evolution of protein function; flavoenzyme; histone demethylation; molecular recognition; Biochemistry, Genetics and Molecular Biology (all)
List of contributors:
Marabelli, Chiara; Marrocco, Biagina; Pilotto, Simona; Chittori, Sagar; Picaud, Sarah; Marchese, Sara; Ciossani, Giuseppe; Forneris, Federico; Filippakopoulos, Panagis; Schoehn, Guy; Rhodes, Daniela; Subramaniam, Sriram; Mattevi, Andrea
Authors of the University:
FORNERIS FEDERICO
MARCHESE SARA
MATTEVI ANDREA
Handle:
https://iris.unipv.it/handle/11571/1259046
Published in:
CELL REPORTS
Journal
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URL

http://www.sciencedirect.com/science/journal/22111247
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