| Literature DB >> 24752549 |
Hee-Jin Jun1, Ji Hae Lee1, Jiyoung Kim1, Yaoyao Jia1, Kyoung Heon Kim1, Kwang Yeon Hwang2, Eun Ju Yun1, Kyoung-Rok Do1, Sung-Joon Lee1.
Abstract
We investigated the hypotriglyceridemic mechanism of action of linalool, an aromatic monoterpene present in teas and fragrant herbs. Reporter gene and time-resolved fluorescence resonance energy transfer assays demonstrated that linalool is a direct ligand of PPARα. Linalool stimulation reduced cellular lipid accumulation regulating PPARα-responsive genes and significantly induced FA oxidation, and its effects were markedly attenuated by silencing PPARα expression. In mice, the oral administration of linalool for 3 weeks reduced plasma TG concentrations in Western-diet-fed C57BL/6J mice (31%, P < 0.05) and human apo E2 mice (50%, P < 0.05) and regulated hepatic PPARα target genes. However, no such effects were seen in PPARα-deficient mice. Transcriptome profiling revealed that linalool stimulation rewired global gene expression in lipid-loaded hepatocytes and that the effects of 1 mM linalool were comparable to those of 0.1 mM fenofibrate. Metabolomic analysis of the mouse plasma revealed that the global metabolite profiles were significantly distinguishable between linalool-fed mice and controls. Notably, the concentrations of saturated FAs were significantly reduced in linalool-fed mice. These findings suggest that the appropriate intake of a natural aromatic compound could exert beneficial metabolic effects by regulating a cellular nutrient sensor.Entities:
Keywords: agonist; linalool; peroxisome proliferator-activated receptor-α; triglyceride
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Year: 2014 PMID: 24752549 PMCID: PMC4031941 DOI: 10.1194/jlr.M045807
Source DB: PubMed Journal: J Lipid Res ISSN: 0022-2275 Impact factor: 5.922