A novel PPARα agonist ameliorates insulin resistance in dogs fed a high-fat diet

被引:24
|
作者
Tsunoda, Masaki [1 ]
Kobayashi, Naoki [1 ]
Ide, Tomohiro [1 ]
Utsumi, Mari [1 ]
Nagasawa, Michiaki [1 ]
Murakami, Koji [1 ]
机构
[1] Kyorin Pharmaceut Co Ltd, Discovery Res Labs, Tochigi 3290114, Japan
来源
AMERICAN JOURNAL OF PHYSIOLOGY-ENDOCRINOLOGY AND METABOLISM | 2008年 / 294卷 / 05期
关键词
KRP-101; obesity; insulin resistance; muscle lipid oxidation;
D O I
10.1152/ajpendo.00627.2007
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
Agonism of peroxisome proliferator-activated receptor (PPAR) alpha, a key regulator of lipid metabolism, leads to amelioration of lipid abnormalities in dyslipidemic patients. However, whether PPAR alpha agonism is an effective form of therapy for obesity-related insulin resistance associated with lipid abnormalities is unclear. The present study investigated the effects of a potent and subtype-selective PPAR alpha agonist, KRP-101, in a nonrodent insulin-resistant animal model under pair-fed conditions. Beagle dogs were fed a high-fat diet for 24 wk to induce insulin resistance. During the final 12 wk, 0.03 mg center dot kg(-1)center dot day(-1) KRP-101 (n = 5) or vehicle (n = 5) was administered orally once a day. KRP-101 administration resulted in a significantly lower weight of overall visceral fat, which is associated with increased adiponectin and decreased leptin in serum. KRP-101 administration improved hyperglycemia and hyperinsulinemia as well as dyslipidemia in dogs fed a high-fat diet. Oral glucose tolerance test showed that KRP-101 administration improved glucose intolerance. The KRP-101 group showed a markedly lower hepatic triglyceride concentration. Lipid oxidation was increased in the liver and skeletal muscles of the KRP-101 group. These findings in the dog model suggest that the use of potent and subtype-selective PPAR alpha agonists as a potentially relevant therapeutic approach to treat human insulin resistance associated with visceral obesity.
引用
收藏
页码:E833 / E840
页数:8
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