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Molecular characterization of new selective peroxisome proliferator-activated receptor γ modulators with angiotensin receptor blocking activity
被引:246
作者:

Schupp, M
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机构: CCM Charite Univ Med Berlin, Inst Pharmacol & Toxicol, Cardiovasc Res Ctr, D-10115 Berlin, Germany

Clemenz, M
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机构: CCM Charite Univ Med Berlin, Inst Pharmacol & Toxicol, Cardiovasc Res Ctr, D-10115 Berlin, Germany

Gineste, R
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机构: CCM Charite Univ Med Berlin, Inst Pharmacol & Toxicol, Cardiovasc Res Ctr, D-10115 Berlin, Germany

Witt, H
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机构: CCM Charite Univ Med Berlin, Inst Pharmacol & Toxicol, Cardiovasc Res Ctr, D-10115 Berlin, Germany

Janke, J
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机构: CCM Charite Univ Med Berlin, Inst Pharmacol & Toxicol, Cardiovasc Res Ctr, D-10115 Berlin, Germany

Helleboid, S
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机构: CCM Charite Univ Med Berlin, Inst Pharmacol & Toxicol, Cardiovasc Res Ctr, D-10115 Berlin, Germany

Hennuyer, N
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机构: CCM Charite Univ Med Berlin, Inst Pharmacol & Toxicol, Cardiovasc Res Ctr, D-10115 Berlin, Germany

Ruiz, P
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机构: CCM Charite Univ Med Berlin, Inst Pharmacol & Toxicol, Cardiovasc Res Ctr, D-10115 Berlin, Germany

Unger, T
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机构: CCM Charite Univ Med Berlin, Inst Pharmacol & Toxicol, Cardiovasc Res Ctr, D-10115 Berlin, Germany

Staels, B
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机构: CCM Charite Univ Med Berlin, Inst Pharmacol & Toxicol, Cardiovasc Res Ctr, D-10115 Berlin, Germany

Kintscher, U
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机构: CCM Charite Univ Med Berlin, Inst Pharmacol & Toxicol, Cardiovasc Res Ctr, D-10115 Berlin, Germany
机构:
[1] CCM Charite Univ Med Berlin, Inst Pharmacol & Toxicol, Cardiovasc Res Ctr, D-10115 Berlin, Germany
[2] GENFIT, Loos, France
[3] Max Planck Inst Mol Genet, Berlin, Germany
[4] Charite Univ Med Berlin, HELIOS Hosp Berlin, Franz Volhard Clin, D-10115 Berlin, Germany
[5] Univ Lille 2, Inst Pasteur Lille, Fac Pharm,Dept Atherosclerose, INSERM,UR 545, Lille, France
来源:
关键词:
D O I:
10.2337/diabetes.54.12.3442
中图分类号:
R5 [内科学];
学科分类号:
1002 ;
100201 ;
摘要:
Selective peroxisome proliferator-activated receptor (PPAR) gamma modulation is a new pharmacological approach that, based on selective receptor-cofactor interactions and target gene regulation, should result in potent insulin sensitization in the absence of PPAR gamma-mediated adverse effects. Here, we characterize two angiotensin receptor blockers (ARBs), telmisartan and irbesartan, as new selective PPAR modulators (SPPARMs). Analysis of PPAR gamma protein conformation using protease protection showed that telmisartan directly interacts with the receptor, producing a distinct conformational change compared with a glitazone. Glutathione S-transferase pull-down and fluorescence resonance energy transfer assays revealed selective cofactor binding by the ARBs compared with glitazones with an attenuated release of the nuclear receptor corepressor and absence of transcriptional intermediary factor 2 recruitment by ARBs. Consistently, selective cofactor binding resulted in differential gene expression profiles in adipocytes (ARB versus glitazone treated) assessed by oligo microarray analysis. Finally, telmisartan improved insulin sensitivity in diet-induced obese mice in the absence of weight gain. The present study identities two ARBs as new SPPARMs. SPPARM activity by ARBs could retain the metabolic efficacy of PPAR gamma activation with reduction in adverse effects exerting in parallel AT1 receptor blockade. This may provide a new therapeutic option for better cardiovascular risk management in metabolic diseases and may initiate the development of new classes of drugs combining potent antihypertensive and antidiabetic actions.
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页码:3442 / 3452
页数:11
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机构: Sahlgrens Univ Hosp, Dept Med, SE-41685 Gothenburg, Sweden