Histone demethylating agents as potential S-adenosyl-l-methionine-competitors

Navakauskiene, R.; Mori, M.; Christodoulou, M.S.; Zentelyte, A.; Botta, B.; Via, L..D.; Ricci, F.; Damia, G.; Passarella, D.; Zilio, C.; Martinet, N.

doi:10.1039/c6md00170j

Histone H3 methylation on K9 and/or K27 depends on histone lysine methyltransferases (KMTs). EZH2, one of the components of the PRC2 complex, catalyzes the trimethylation of histone H3K27, which is associated with transcriptional repression and tumor development. H3K9me3 mediated gene silencing may result from other KDMs such as G9a/GLP, SUV39H1-2, SETDB1, CCLD8 and RIZ1. Their disturbance leads to defective cell mitosis. It is therefore desirable to find small molecules that are able to decrease H3K9 and K27 tagging to reinitiate gene transcription. Most KDM inhibitors are still based on SAM co-factor competition/modulation. Herein, functional screening of a diversity library proved to be a useful tool for finding new specific KDM inhibitors; the use of SAM-based pharmacophoric models facilitated the understanding of their possible mechanism of action.

Histone demethylating agents as potential S-adenosyl-l-methionine-competitors / R. Navakauskiene, M. Mori, M.S. Christodoulou, A. Zentelyte, B. Botta, L..D. Via, F. Ricci, G. Damia, D. Passarella, C. Zilio, N. Martinet. - In: MEDCHEMCOMM. - ISSN 2040-2503. - 7:6(2016), pp. 1245-1255. [10.1039/c6md00170j]

Histone demethylating agents as potential S-adenosyl-l-methionine-competitors

R. Navakauskiene;M. Mori;M.S. Christodoulou;A. Zentelyte;B. Botta;L. . D. Via;F. Ricci;G. Damia;D. Passarella;C. Zilio^Penultimo;N. Martinet

2016

Abstract

Histone H3 methylation on K9 and/or K27 depends on histone lysine methyltransferases (KMTs). EZH2, one of the components of the PRC2 complex, catalyzes the trimethylation of histone H3K27, which is associated with transcriptional repression and tumor development. H3K9me3 mediated gene silencing may result from other KDMs such as G9a/GLP, SUV39H1-2, SETDB1, CCLD8 and RIZ1. Their disturbance leads to defective cell mitosis. It is therefore desirable to find small molecules that are able to decrease H3K9 and K27 tagging to reinitiate gene transcription. Most KDM inhibitors are still based on SAM co-factor competition/modulation. Herein, functional screening of a diversity library proved to be a useful tool for finding new specific KDM inhibitors; the use of SAM-based pharmacophoric models facilitated the understanding of their possible mechanism of action.

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	Parole chiave
	
				biochemistry; 3003
			
	Settori scientifico-disciplinari dell'articolo (sola visualizzazione)
	
				Settore CHIM/06 - Chimica Organica
Settore CHIM/08 - Chimica Farmaceutica
			
	Data di pubblicazione
	
				2016
			
	Rivista in ANCE
	
				MEDCHEMCOMM
			
	DOI
	
				https://dx.doi.org/10.1039/c6md00170j
			
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				Article (author)
			
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				01 - Articolo su periodico

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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2434/437336

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