Fracchiolla Giuseppe, Laghezza Antonio, Piemontese Luca, Carbonara Giuseppe, Lavecchia Antonio, Tortorella Paolo, Crestani Maurizio, Novellino Ettore, Loiodice Fulvio
Dipartimento Farmaco-Chimico, Università degli Studi di Bari via Orabona 4, 70126 Bari, Italy.
ChemMedChem. 2007 May;2(5):641-54. doi: 10.1002/cmdc.200600307.
Peroxisome proliferator-activated receptors (PPARs) are ligand-activated transcription factors that govern lipid and glucose homeostasis, and play a central role in cardiovascular disease, obesity, and diabetes. Thus, there is significant interest in developing new and specific agonists for these receptors. Herein we present screening results for a series of chiral phenoxyacetic acid analogues, some of which are potent PPARalpha agonists as well as PPARgamma agonists. The stereochemistry of these compounds plays an important role in determining their activity; the S isomers were observed to be more active than the corresponding R isomers. Interestingly, for one of these analogues, the stereoselectivity toward PPARalpha was reversed, and for this reason docking experiments were performed to rationalize this peculiar behavior.
过氧化物酶体增殖物激活受体(PPARs)是配体激活的转录因子,调控脂质和葡萄糖稳态,在心血管疾病、肥胖症和糖尿病中起核心作用。因此,开发针对这些受体的新型特异性激动剂备受关注。在此,我们展示了一系列手性苯氧乙酸类似物的筛选结果,其中一些是强效的PPARα激动剂以及PPARγ激动剂。这些化合物的立体化学在决定其活性方面起着重要作用;观察到S异构体比相应的R异构体更具活性。有趣的是,对于其中一种类似物,其对PPARα的立体选择性发生了反转,因此进行了对接实验以解释这种特殊行为。
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