Leptin controls adipose tissue lipogenesis via central, STAT3–independent mechanisms

被引:0
|
作者
Christoph Buettner
Evan D Muse
Andrew Cheng
Linghong Chen
Thomas Scherer
Alessandro Pocai
Kai Su
Bob Cheng
Xiasong Li
Judith Harvey-White
Gary J Schwartz
George Kunos
Luciano Rossetti
机构
[1] Mount Sinai School of Medicine,Department of Medicine
[2] One Gustave L. Levy Place,Department of Molecular Pharmacology
[3] Box 1005,Department of Medicine
[4] Albert Einstein College of Medicine,undefined
[5] Albert Einstein College of Medicine,undefined
[6] Diabetes Research and Training Center,undefined
[7] Albert Einstein College of Medicine,undefined
[8] US National Institute on Alcohol Abuse & Alcoholism,undefined
[9] US National Institutes of Health,undefined
[10] Current address: Merck,undefined
[11] 126 East Lincoln Avenue,undefined
[12] Rahway,undefined
[13] New Jersey 07065,undefined
[14] USA.,undefined
来源
Nature Medicine | 2008年 / 14卷
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摘要
Leptin (encoded by Lep) controls body weight by regulating food intake and fuel partitioning. Obesity is characterized by leptin resistance and increased endocannabinoid tone. Here we show that leptin infused into the mediobasal hypothalamus (MBH) of rats inhibits white adipose tissue (WAT) lipogenesis, which occurs independently of signal transducer and activator of transcription-3 (STAT3) signaling. Correspondingly, transgenic inactivation of STAT3 signaling by mutation of the leptin receptor (s/s mice) leads to reduced adipose mass compared to db/db mice (complete abrogation of leptin receptor signaling). Conversely, the ability of hypothalamic leptin to suppress WAT lipogenesis in rats is lost when hypothalamic phosphoinositide 3-kinase signaling is prevented or when sympathetic denervation of adipose tissue is performed. MBH leptin suppresses the endocannabinoid anandamide in WAT, and, when this suppression of endocannabinoid tone is prevented by systemic CB1 receptor activation, MBH leptin fails to suppress WAT lipogenesis. These data suggest that the increased endocannabinoid tone observed in obesity is linked to a failure of central leptin signaling to restrain peripheral endocannabinoids.
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页码:667 / 675
页数:8
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