A Unique PPARγ Ligand with Potent Insulin-Sensitizing yet Weak Adipogenic Activity

FMOC-L-Leucine (F-L-Leu) is a chemically distinct PPARγ ligand. Two molecules of F-L-Leu bind to the ligand binding domain of a single PPARγ molecule, making its mode of receptor interaction distinct from that of other nuclear receptor ligands. F-L-Leu induces a particular allosteric configuration o...

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Veröffentlicht in:Molecular cell 2001-10, Vol.8 (4), p.737-747
Hauptverfasser: Rocchi, Stéphane, Picard, Frédéric, Vamecq, Joseph, Gelman, Laurent, Potier, Noelle, Zeyer, Denis, Dubuquoy, Laurent, Bac, Pierre, Champy, Marie-France, Plunket, Kelli D., Leesnitzer, Lisa M., Blanchard, Steven G., Desreumaux, Pierre, Moras, Dino, Renaud, Jean-Paul, Auwerx, Johan
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container_issue 4
container_start_page 737
container_title Molecular cell
container_volume 8
creator Rocchi, Stéphane
Picard, Frédéric
Vamecq, Joseph
Gelman, Laurent
Potier, Noelle
Zeyer, Denis
Dubuquoy, Laurent
Bac, Pierre
Champy, Marie-France
Plunket, Kelli D.
Leesnitzer, Lisa M.
Blanchard, Steven G.
Desreumaux, Pierre
Moras, Dino
Renaud, Jean-Paul
Auwerx, Johan
description FMOC-L-Leucine (F-L-Leu) is a chemically distinct PPARγ ligand. Two molecules of F-L-Leu bind to the ligand binding domain of a single PPARγ molecule, making its mode of receptor interaction distinct from that of other nuclear receptor ligands. F-L-Leu induces a particular allosteric configuration of PPARγ, resulting in differential cofactor recruitment and translating in distinct pharmacological properties. F-L-Leu activates PPARγ with a lower potency, but a similar maximal efficacy, than rosiglitazone. The particular PPARγ configuration induced by F-L-Leu leads to a modified pattern of target gene activation. F-L-Leu improves insulin sensitivity in normal, dietinduced 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 PPARγ modulator that activates some (insulin sensitization), but not all (adipogenesis), PPARγ-signaling pathways.
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subjects Analytical chemistry
Chemical Sciences
title A Unique PPARγ Ligand with Potent Insulin-Sensitizing yet Weak Adipogenic Activity
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