CRTC3 links catecholamine signalling to energy balance

The adipose-derived hormone leptin maintains energy balance in part through central nervous system-mediated increases in sympathetic outflow that enhance fat burning. Triggering of β-adrenergic receptors in adipocytes stimulates energy expenditure by cyclic AMP (cAMP)-dependent increases in lipolysi...

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Published in	Nature (London) Vol. 468; no. 7326; pp. 933 - 939
Main Authors	Song, Youngsup, Altarejos, Judith, Goodarzi, Mark O., Inoue, Hiroshi, Guo, Xiuqing, Berdeaux, Rebecca, Kim, Jeong-Ho, Goode, Jason, Igata, Motoyuki, Paz, Jose C., Hogan, Meghan F., Singh, Pankaj K., Goebel, Naomi, Vera, Lili, Miller, Nina, Cui, Jinrui, Jones, Michelle R., Consortium, CHARGE, Consortium, GIANT, Chen, Yii-Der I., Taylor, Kent D., Hsueh, Willa A., Rotter, Jerome I., Montminy, Marc
Format	Journal Article
Language	English
Published	London Nature Publishing Group UK 16.12.2010 Nature Publishing Group
Subjects	631/443/319/333/1465 631/45/612/822 631/80/86/820 692/699/2743/393 Adipocytes - drug effects Adipocytes - metabolism Adipose tissue Adipose Tissue - drug effects Adipose Tissue - metabolism Adipose tissues Animals Bioenergetics Biological and medical sciences Body Temperature Catecholamines Catecholamines - metabolism Cells, Cultured Central nervous system Cyclic AMP - metabolism Cyclic AMP Response Element-Binding Protein - antagonists & inhibitors Cyclic AMP Response Element-Binding Protein - metabolism Dietary Fats - pharmacology Energy balance Energy metabolism Energy Metabolism - genetics Female Genome-Wide Association Study Health aspects Hormones Humanities and Social Sciences Humans Insulin Resistance Leptin Medical sciences Metabolic diseases Mexican Americans - genetics Mice multidisciplinary Obesity Obesity - chemically induced Obesity - genetics Obesity - metabolism Phosphorylation Properties Receptors, Adrenergic, beta - metabolism RGS Proteins - biosynthesis RGS Proteins - genetics Science Science (multidisciplinary) Signal transduction Signal Transduction - drug effects Signal Transduction - physiology Transcription Factors - chemistry Transcription Factors - deficiency Transcription Factors - genetics Transcription Factors - metabolism Transcriptional coactivators United States Obesity Leptin Knockout mouse Adipokine Catecholamine Transcription factor CREB β-Adrenergic receptor
Online Access	Get full text
ISSN	0028-0836 1476-4687 1476-4687
DOI	10.1038/nature09564

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Abstract	The adipose-derived hormone leptin maintains energy balance in part through central nervous system-mediated increases in sympathetic outflow that enhance fat burning. Triggering of β-adrenergic receptors in adipocytes stimulates energy expenditure by cyclic AMP (cAMP)-dependent increases in lipolysis and fatty-acid oxidation. Although the mechanism is unclear, catecholamine signalling is thought to be disrupted in obesity, leading to the development of insulin resistance. Here we show that the cAMP response element binding (CREB) coactivator Crtc3 promotes obesity by attenuating β-adrenergic receptor signalling in adipose tissue. Crtc3 was activated in response to catecholamine signals, when it reduced adenyl cyclase activity by upregulating the expression of Rgs2 , a GTPase-activating protein that also inhibits adenyl cyclase activity. As a common human CRTC3 variant with increased transcriptional activity is associated with adiposity in two distinct Mexican-American cohorts, these results suggest that adipocyte CRTC3 may play a role in the development of obesity in humans. CRTC3 protein linked to obesity The cyclic-AMP-responsive protein Crtc3 (CREB-regulated transcription coactivator 3) is shown to promote obesity and insulin resistance in mice on high-fat diets by attenuating β-adrenergic receptor signalling in adipocytes. Crtc3 is expressed predominantly in adipose tissue; mice lacking Crtc3 are protected from the development of diet-induced obesity and remain insulin sensitive. This work suggests that Crtc3 may be an early signal in the development of obesity and perhaps also in type II diabetes. β-adrenergic receptor signalling in adipocytes stimulates energy expenditure via cAMP-dependent increases in lipolysis and fatty-acid oxidation, and this signalling mechanism is thought to be disrupted in obesity. Here, the cAMP-responsive CREB coactivator Crtc3 is shown to promote obesity in mice by attenuating β adrenergic receptor signalling in adipose tissue.
AbstractList	The adipose-derived hormone leptin maintains energy balance in part through central nervous system-mediated increases in sympathetic outflow that enhance fat burning. Triggering of β-adrenergic receptors in adipocytes stimulates energy expenditure by cyclic AMP (cAMP)-dependent increases in lipolysis and fatty-acid oxidation. Although the mechanism is unclear, catecholamine signalling is thought to be disrupted in obesity, leading to the development of insulin resistance. Here we show that the cAMP response element binding (CREB) coactivator Crtc3 promotes obesity by attenuating β-adrenergic receptor signalling in adipose tissue. Crtc3 was activated in response to catecholamine signals, when it reduced adenyl cyclase activity by upregulating the expression of Rgs2 , a GTPase-activating protein that also inhibits adenyl cyclase activity. As a common human CRTC3 variant with increased transcriptional activity is associated with adiposity in two distinct Mexican-American cohorts, these results suggest that adipocyte CRTC3 may play a role in the development of obesity in humans. CRTC3 protein linked to obesity The cyclic-AMP-responsive protein Crtc3 (CREB-regulated transcription coactivator 3) is shown to promote obesity and insulin resistance in mice on high-fat diets by attenuating β-adrenergic receptor signalling in adipocytes. Crtc3 is expressed predominantly in adipose tissue; mice lacking Crtc3 are protected from the development of diet-induced obesity and remain insulin sensitive. This work suggests that Crtc3 may be an early signal in the development of obesity and perhaps also in type II diabetes. β-adrenergic receptor signalling in adipocytes stimulates energy expenditure via cAMP-dependent increases in lipolysis and fatty-acid oxidation, and this signalling mechanism is thought to be disrupted in obesity. Here, the cAMP-responsive CREB coactivator Crtc3 is shown to promote obesity in mice by attenuating β adrenergic receptor signalling in adipose tissue. The adipose-derived hormone leptin maintains energy balance in part through central nervous system-mediated increases in sympathetic outflow that enhance fat burning. Triggering of β-adrenergic receptors in adipocytes stimulates energy expenditure by cyclic AMP (cAMP)-dependent increases in lipolysis and fatty-acid oxidation. Although the mechanism is unclear, catecholamine signalling is thought to be disrupted in obesity, leading to the development of insulin resistance. Here we show that the cAMP response element binding (CREB) coactivator Crtc3 promotes obesity by attenuating β-adrenergic receptor signalling in adipose tissue. Crtc3 was activated in response to catecholamine signals, when it reduced adenyl cyclase activity by upregulating the expression of Rgs2, a GTPase-activating protein that also inhibits adenyl cyclase activity. As a common human CRTC3 variant with increased transcriptional activity is associated with adiposity in two distinct Mexican-American cohorts, these results suggest that adipocyte CRTC3 may play a role in the development of obesity in humans. The adipose-derived hormone leptin maintains energy balance in part through central nervous system-mediated increases in sympathetic outflow that enhance fat burning. Triggering of β-adrenergic receptors in adipocytes stimulates energy expenditure by cyclic AMP (cAMP)-dependent increases in lipolysis and fatty-acid oxidation. Although the mechanism is unclear, catecholamine signalling is thought to be disrupted in obesity, leading to the development of insulin resistance. Here we show that the cAMP response element binding (CREB) coactivator Crtc3 promotes obesity by attenuating β-adrenergic receptor signalling in adipose tissue. Crtc3 was activated in response to catecholamine signals, when it reduced adenyl cyclase activity by upregulating the expression of Rgs2, a GTPase-activating protein that also inhibits adenyl cyclase activity. As a common human CRTC3 variant with increased transcriptional activity is associated with adiposity in two distinct Mexican-American cohorts, these results suggest that adipocyte CRTC3 may play a role in the development of obesity in humans.The adipose-derived hormone leptin maintains energy balance in part through central nervous system-mediated increases in sympathetic outflow that enhance fat burning. Triggering of β-adrenergic receptors in adipocytes stimulates energy expenditure by cyclic AMP (cAMP)-dependent increases in lipolysis and fatty-acid oxidation. Although the mechanism is unclear, catecholamine signalling is thought to be disrupted in obesity, leading to the development of insulin resistance. Here we show that the cAMP response element binding (CREB) coactivator Crtc3 promotes obesity by attenuating β-adrenergic receptor signalling in adipose tissue. Crtc3 was activated in response to catecholamine signals, when it reduced adenyl cyclase activity by upregulating the expression of Rgs2, a GTPase-activating protein that also inhibits adenyl cyclase activity. As a common human CRTC3 variant with increased transcriptional activity is associated with adiposity in two distinct Mexican-American cohorts, these results suggest that adipocyte CRTC3 may play a role in the development of obesity in humans. The adipose-derived hormone leptin maintains energy balance in part through central nervous system-mediated increases in sympathetic outflow that enhance fat burning. Triggering of β-adrenergic receptors in adipocytes stimulates energy expenditure by cyclic AMP (cAMP)-dependent increases in lipolysis and fatty-acid oxidation. Although the mechanism is unclear, catecholamine signalling is thought to be disrupted in obesity, leading to the development of insulin resistance. Here we show that the cAMP response element binding (CREB) coactivator Crtc3 promotes obesity by attenuating β-adrenergic receptor signalling in adipose tissue. Crtc3 was activated in response to catecholamine signals, when it reduced adenyl cyclase activity by upregulating the expression of Rgs2, a GTPase-activating protein that also inhibits adenyl cyclase activity. As a common human CRTC3 variant with increased transcriptional activity is associated with adiposity in two distinct Mexican-American cohorts, these results suggest that adipocyte CRTC3 may play a role in the development of obesity in humans. [PUBLICATION ABSTRACT]
Audience	Academic
Author	Altarejos, Judith Guo, Xiuqing Goebel, Naomi Goodarzi, Mark O. Vera, Lili Igata, Motoyuki Singh, Pankaj K. Inoue, Hiroshi Montminy, Marc Kim, Jeong-Ho Rotter, Jerome I. Hogan, Meghan F. Taylor, Kent D. Consortium, CHARGE Jones, Michelle R. Cui, Jinrui Consortium, GIANT Goode, Jason Paz, Jose C. Berdeaux, Rebecca Miller, Nina Hsueh, Willa A. Chen, Yii-Der I. Song, Youngsup
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Copyright	Springer Nature Limited 2010 2015 INIST-CNRS COPYRIGHT 2010 Nature Publishing Group Copyright Nature Publishing Group Dec 16, 2010
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Keywords	Obesity Leptin Knockout mouse Adipokine Catecholamine Transcription factor CREB β-Adrenergic receptor
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Snippet	The adipose-derived hormone leptin maintains energy balance in part through central nervous system-mediated increases in sympathetic outflow that enhance fat...
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Title	CRTC3 links catecholamine signalling to energy balance
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