Side-Chain Modified Ergosterol and Stigmasterol Derivatives as Liver X Receptor Agonists

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A series of stigmasterol and ergosterol derivatives, characterized by the presence of oxygenated functions at C-22 and/or C-23 positions, were designed as potential liver X receptor (LXR) agonists. The absolute configuration of the newly created chiral centers was definitively assigned for all the corresponding compounds. Among the 16 synthesized compounds, 21, 27, and 28 were found to be selective LXRÎ± agonists, whereas 20, 22, and 25 showed good selectivity for the LXRÎ² isoform. In particular, 25 showed the same degree of potency as 22R-HC (3) at LXRÎ², while it was virtually inactive at LXRÎ± (EC50 = 14.51 Î¼M). Interestingly, 13, 19, 20, and 25 showed to be LXR target gene-selective modulators, by strongly inducing the expression of ABCA1, while poorly or not activating the lipogenic genes SREBP1 and SCD1 or FASN, respectively.

Marinozzi, M., Castro Navas, F.F., Maggioni, D., Carosati, E., Bocci, G., Carloncelli, M., et al. (2017). Side-Chain Modified Ergosterol and Stigmasterol Derivatives as Liver X Receptor Agonists. JOURNAL OF MEDICINAL CHEMISTRY, 60(15), 6548-6562 [10.1021/acs.jmedchem.7b00091].

Side-Chain Modified Ergosterol and Stigmasterol Derivatives as Liver X Receptor Agonists

Marinozzi, Maura;Castro Navas, Francisco Fermin;Maggioni, Daniela;Carosati, Emanuele;Bocci, Giovanni;Carloncelli, Maria;GIORGI, GIANLUCA;Cruciani, Gabriele;Fontana, Raffaella;Russo, Vincenzo

2017-01-01

Abstract

A series of stigmasterol and ergosterol derivatives, characterized by the presence of oxygenated functions at C-22 and/or C-23 positions, were designed as potential liver X receptor (LXR) agonists. The absolute configuration of the newly created chiral centers was definitively assigned for all the corresponding compounds. Among the 16 synthesized compounds, 21, 27, and 28 were found to be selective LXRÎ± agonists, whereas 20, 22, and 25 showed good selectivity for the LXRÎ² isoform. In particular, 25 showed the same degree of potency as 22R-HC (3) at LXRÎ², while it was virtually inactive at LXRÎ± (EC50 = 14.51 Î¼M). Interestingly, 13, 19, 20, and 25 showed to be LXR target gene-selective modulators, by strongly inducing the expression of ABCA1, while poorly or not activating the lipogenic genes SREBP1 and SCD1 or FASN, respectively.

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	Anno
	
				2017
			
	Rivista su cui è pubblicata l'opera
	
				JOURNAL OF MEDICINAL CHEMISTRY
			
	Citazione
	
				Marinozzi, M., Castro Navas, F.F., Maggioni, D., Carosati, E., Bocci, G., Carloncelli, M., et al. (2017). Side-Chain Modified Ergosterol and Stigmasterol Derivatives as Liver X Receptor Agonists. JOURNAL OF MEDICINAL CHEMISTRY, 60(15), 6548-6562 [10.1021/acs.jmedchem.7b00091].
			
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11365/1030439