21862615

Source:http://linkedlifedata.com/resource/pubmed/id/21862615

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Predicate	Object
rdf:type	pubmed:Citation
lifeskim:mentions	umls-concept:C0021641, umls-concept:C0021665, umls-concept:C0132096, umls-concept:C0851285, umls-concept:C1325969, umls-concept:C1704259, umls-concept:C1705987
pubmed:issue	10
pubmed:dateCreated	2011-9-22
pubmed:abstractText	Brown adipose tissue plays an important role in obesity, insulin resistance, and diabetes. We have previously shown that the transition from brown preadipocytes to mature adipocytes is mediated in part by insulin receptor substrate (IRS)-1 and the cell cycle regulator protein necdin. In this study, we used pharmacological inhibitors and adenoviral dominant negative constructs to demonstrate that this transition involves IRS-1 activation of Ras and ERK1/2, resulting in phosphorylation of cAMP response element-binding protein (CREB) and suppression of necdin expression. This signaling did not include an elevation of intracellular calcium. A constitutively active form of CREB expressed in IRS-1 knockout cells decreased necdin promoter activity, necdin mRNA, and necdin protein levels, leading to a partial restoration of differentiation. By contrast, forkhead box protein (Fox)O1, which is regulated by the phosphoinositide 3 kinase-Akt pathway, increased necdin promoter activity. Based on reporter gene assays using truncations of the necdin promoter and chromatin immunoprecipitation studies, we demonstrated that CREB and FoxO1 are recruited to the necdin promoter, likely interacting with specific consensus sequences in the proximal region. Based on these results, we propose that insulin/IGF-I act through IRS-1 phosphorylation to stimulate differentiation of brown preadipocytes via two complementary pathways: 1) the Ras-ERK1/2 pathway to activate CREB and 2) the phosphoinositide 3 kinase-Akt pathway to deactivate FoxO1. These two pathways combine to decrease necdin levels and permit the clonal expansion and coordinated gene expression necessary to complete brown adipocyte differentiation.
pubmed:grant	http://linkedlifedata.com/resource/pubmed/grant/DK046200, http://linkedlifedata.com/resource/pubmed/grant/DK070722, http://linkedlifedata.com/resource/pubmed/grant/DK077097, http://linkedlifedata.com/resource/pubmed/grant/DK081604, http://linkedlifedata.com/resource/pubmed/grant/DK087317, http://linkedlifedata.com/resource/pubmed/grant/DK33201, http://linkedlifedata.com/resource/pubmed/grant/DK41430, http://linkedlifedata.com/resource/pubmed/grant/P30 DK040561, http://linkedlifedata.com/resource/pubmed/grant/P30 DK46200, http://linkedlifedata.com/resource/pubmed/grant/RR025757
pubmed:language	eng
pubmed:journal	http://linkedlifedata.com/resource/pubmed/journal/0375040
pubmed:citationSubset	AIM
pubmed:chemical	http://linkedlifedata.com/resource/pubmed/chemical/Creb1 protein, mouse, http://linkedlifedata.com/resource/pubmed/chemical/Cyclic AMP Response..., http://linkedlifedata.com/resource/pubmed/chemical/Extracellular Signal-Regulated MAP..., http://linkedlifedata.com/resource/pubmed/chemical/Forkhead Transcription Factors, http://linkedlifedata.com/resource/pubmed/chemical/Foxo1 protein, mouse, http://linkedlifedata.com/resource/pubmed/chemical/Insulin, http://linkedlifedata.com/resource/pubmed/chemical/Insulin Receptor Substrate Proteins, http://linkedlifedata.com/resource/pubmed/chemical/Insulin-Like Growth Factor I, http://linkedlifedata.com/resource/pubmed/chemical/Irs1 protein, mouse, http://linkedlifedata.com/resource/pubmed/chemical/Nerve Tissue Proteins, http://linkedlifedata.com/resource/pubmed/chemical/Nuclear Proteins, http://linkedlifedata.com/resource/pubmed/chemical/necdin
pubmed:status	MEDLINE
pubmed:month	Oct
pubmed:issn	1945-7170
pubmed:author	pubmed-author:CypessAaron MAM, pubmed-author:EspinozaDaniel ODO, pubmed-author:HuangTian LianTL, pubmed-author:KristiansenKarstenK, pubmed-author:SchulzTim JTJ, pubmed-author:TsengYu-HuaYH, pubmed-author:UntermanTerry GTG, pubmed-author:ZhangHongbinH
pubmed:issnType	Electronic
pubmed:volume	152
pubmed:owner	NLM
pubmed:authorsComplete	Y
pubmed:pagination	3680-9
pubmed:dateRevised	2011-11-17
pubmed:meshHeading	pubmed-meshheading:21862615-Adipocytes, Brown, pubmed-meshheading:21862615-Adipogenesis, pubmed-meshheading:21862615-Animals, pubmed-meshheading:21862615-Cell Differentiation, pubmed-meshheading:21862615-Cells, Cultured, pubmed-meshheading:21862615-Cyclic AMP Response Element-Binding Protein, pubmed-meshheading:21862615-Extracellular Signal-Regulated MAP Kinases, pubmed-meshheading:21862615-Forkhead Transcription Factors, pubmed-meshheading:21862615-Insulin, pubmed-meshheading:21862615-Insulin Receptor Substrate Proteins, pubmed-meshheading:21862615-Insulin-Like Growth Factor I, pubmed-meshheading:21862615-Mice, pubmed-meshheading:21862615-Nerve Tissue Proteins, pubmed-meshheading:21862615-Nuclear Proteins, pubmed-meshheading:21862615-Phosphorylation, pubmed-meshheading:21862615-Promoter Regions, Genetic, pubmed-meshheading:21862615-Signal Transduction
pubmed:year	2011
pubmed:articleTitle	Insulin/IGF-I regulation of necdin and brown adipocyte differentiation via CREB- and FoxO1-associated pathways.
pubmed:affiliation	Research Division, Joslin Diabetes Center, Department of Medicine, Harvard Medical School, Boston, Massachusetts 02215, USA. aaron.cypess@joslin.harvard.edu
pubmed:publicationType	Journal Article, Research Support, U.S. Gov't, Non-P.H.S., Research Support, Non-U.S. Gov't, Research Support, N.I.H., Extramural