Literature DB >> 11684010

A unique PPARgamma ligand with potent insulin-sensitizing yet weak adipogenic activity.

S Rocchi1, F Picard, J Vamecq, L Gelman, N Potier, D Zeyer, L Dubuquoy, P Bac, M F Champy, K D Plunket, L M Leesnitzer, S G Blanchard, P Desreumaux, D Moras, J P Renaud, J Auwerx.   

Abstract

FMOC-L-Leucine (F-L-Leu) is a chemically distinct PPARgamma ligand. Two molecules of F-L-Leu bind to the ligand binding domain of a single PPARgamma molecule, making its mode of receptor interaction distinct from that of other nuclear receptor ligands. F-L-Leu induces a particular allosteric configuration of PPARgamma, resulting in differential cofactor recruitment and translating in distinct pharmacological properties. F-L-Leu activates PPARgamma with a lower potency, but a similar maximal efficacy, than rosiglitazone. The particular PPARgamma configuration induced by F-L-Leu leads to a modified pattern of target gene activation. F-L-Leu improves insulin sensitivity in normal, diet-induced glucose-intolerant, and in diabetic db/db mice, yet it has a lower adipogenic activity. These biological effects suggest that F-L-Leu is a selective PPARgamma modulator that activates some (insulin sensitization), but not all (adipogenesis), PPARgamma-signaling pathways.

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Year:  2001        PMID: 11684010     DOI: 10.1016/s1097-2765(01)00353-7

Source DB:  PubMed          Journal:  Mol Cell        ISSN: 1097-2765            Impact factor:   17.970


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