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Structural basis of LSD1-CoREST selectivity in histone H3 recognition

Articolo
Data di Pubblicazione:
2007
Citazione:
Structural basis of LSD1-CoREST selectivity in histone H3 recognition / F. Forneris, C. Binda, A. Adamo, E. Battaglioli, A. Mattevi. - In: THE JOURNAL OF BIOLOGICAL CHEMISTRY. - ISSN 0021-9258. - 282:28(2007 Jul 13), pp. 20070-20074.
Abstract:
Histone demethylase LSD1 regulates transcription by demethylating Lys(4) of histone H3. The crystal structure of the enzyme in complex with CoREST and a substrate-like peptide inhibitor highlights an intricate network of interactions and a folded conformation of the bound peptide. The core of the peptide structure is formed by Arg(2), Gln(5), and Ser(10), which are engaged in specific intramolecular H-bonds. Several charged side chains on the surface of the substrate-binding pocket establish electrostatic interactions with the peptide. The three-dimensional structure predicts that methylated Lys(4) binds in a solvent inaccessible position in front of the flavin cofactor. This geometry is fully consistent with the demethylation reaction being catalyzed through a flavin-mediated oxidation of the substrate amino-methyl group. These features dictate the exquisite substrate specificity of LSD1 and provide a structural framework to explain the fine tuning of its catalytic activity and the active role of CoREST in substrate recognition.
Tipologia IRIS:
01 - Articolo su periodico
Elenco autori:
F. Forneris, C. Binda, A. Adamo, E. Battaglioli, A. Mattevi
Autori di Ateneo:
BATTAGLIOLI ELENA ( autore )
Link alla scheda completa:
https://air.unimi.it/handle/2434/42863
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