Sulfonylthiadiazoles with an unusual binding mode as partial dual peroxisome proliferator-activated receptor (PPAR) γ/δ agonists with high potency and in vivo efficacy

Stefanie Keil; Hans Matter; Karl Schönafinger; Maike Glien; Magali Mathieu; Jean-Pierre Marquette; Nadine Michot; Silke Haag-Diergarten; Matthias Urmann; Wolfgang Wendler

doi:10.1002/cmdc.201100047

Sulfonylthiadiazoles with an unusual binding mode as partial dual peroxisome proliferator-activated receptor (PPAR) γ/δ agonists with high potency and in vivo efficacy

ChemMedChem. 2011 Apr 4;6(4):633-53. doi: 10.1002/cmdc.201100047. Epub 2011 Mar 11.

Authors

Stefanie Keil¹, Hans Matter, Karl Schönafinger, Maike Glien, Magali Mathieu, Jean-Pierre Marquette, Nadine Michot, Silke Haag-Diergarten, Matthias Urmann, Wolfgang Wendler

Affiliation

¹ Sanofi-Aventis Deutschland GmbH, R&D, Diabetes Division and Lead Generation & Candidate Realization, Industriepark Hoechst, Building G 878, 65926 Frankfurt am Main, Germany. stefanie.keil@sanofi-aventis.com

PMID: 21400663
DOI: 10.1002/cmdc.201100047

Abstract

Compounds that simultaneously activate the peroxisome proliferator-activated receptor (PPAR) subtypes PPARγ and PPARδ have the potential to effectively target dyslipidemia and type II diabetes in a single pharmaceutically active molecule. The frequently observed side effects of selective PPARγ agonists, such as edema and weight gain, are expected to be overcome by using partial instead of full agonists for this nuclear receptor family. Herein we report the discovery, synthesis, and optimization of a novel series of sulfonylthiadiazoles that are active as partial agonists. The initial compound 6 was discovered by high-throughput screening as a moderate partial PPARδ agonist; its optimization was based on the X-ray crystal structure in complex with PPARδ. In contrast to other PPARδ agonists, this ligand does not interact directly with residues from the activation helix AF-2, which might be linked to its partial agonistic effect. Interestingly, the thiadiazole moiety fills a novel subpocket, which becomes accessible after moderate conformational rearrangement. The optimization was focused on introducing conformational constraints and replacing intramolecular hydrogen bonding interactions. Highly potent molecules with activity as dual partial PPARγ/δ agonists in the low nanomolar range were then identified. One of the most active members, compound 20 a, displayed EC₅₀ values of 1.6 and 336 nM for PPARδ and γ, respectively. The X-ray crystal structure of its complex with PPARδ confirms our design hypothesis. Compound 20 a clearly displayed in vivo activity in two chronic mice studies. Lipids were modified in a beneficial way in normolipidemic mice, and the development of overt diabetes could be prevented in pre-diabetic db/db mice. However, body weight gain was similar to that observed with the PPARγ agonist rosiglitazone. Hence, active compounds from this series can be considered as valuable tools to elucidate the complex roles of dual PPARγ/δ agonists for potential treatment of metabolic syndrome.

MeSH terms

Animals
Binding Sites
Crystallography, X-Ray
Diabetes Mellitus, Experimental / drug therapy
Diabetes Mellitus, Experimental / metabolism
Diabetes Mellitus, Experimental / pathology
Diabetes Mellitus, Type 2 / drug therapy
Diabetes Mellitus, Type 2 / metabolism
Diabetes Mellitus, Type 2 / pathology
Mice
PPAR delta / agonists*
PPAR delta / metabolism
PPAR gamma / agonists*
PPAR gamma / metabolism
Structure-Activity Relationship
Sulfones / agonists
Sulfones / chemical synthesis
Sulfones / chemistry
Sulfones / therapeutic use*
Thiadiazoles / agonists
Thiadiazoles / chemical synthesis
Thiadiazoles / chemistry
Thiadiazoles / therapeutic use*

Substances

PPAR delta
PPAR gamma
Sulfones
Thiadiazoles