A Novel Regulatory Pathway of Brown Fat Thermogenesis

Mauri, Teresa; Andrés, Javier De; Yubero, Pilar; Viñas, Octavi; Mampel, Teresa; Iglesias, Roser; Giralt, Marta; Villarroya, Francesc

doi:10.1074/jbc.270.10.5666

Cited by 182 publications

(117 citation statements)

References 50 publications

Supporting

Mentioning

110

Contrasting

Order By: Relevance

“…10 Wg RNA was used for Northern blot analysis, as reported [9]. For detection of PhyH mRNA, a probe was obtained after coupled reverse transcription and PCR ampli¢cation of mouse liver RNA using the primers 5P-GCAGTTTCGTCTGCTG-GCC-3P and 5P-GTACCTCACTCTTGAAGGGC-3P, which correspond to positions 14^29 and 1080^1061 in the PhyH cDNA sequence (GenBank AF023463).…”

Section: Methodsmentioning

confidence: 99%

Phytanic acid, but not pristanic acid, mediates the positive effects of phytol derivatives on brown adipocyte differentiation

et al. 2002

Self Cite

View full text Add to dashboard Cite

The phytol derivatives phytanic acid and pristanic acid may activate nuclear hormone receptors and influence gene expression and cell differentiation. Phytanic acid induces brown adipocyte differentiation. It was determined that brown fat and brown adipocytes are sites of high gene expression of phytanoylCoA hydroxylase, the enzyme required for initiation of peroxisomal K K-oxidation of phytanic acid. However, the effects of phytanic acid were not mediated by its K K-oxidation product pristanic acid, which did not promote brown adipocyte differentiation or stimulate transcription of the uncoupling protein-1 gene. Moreover, acute cold exposure of mice caused a dramatic mobilization of the phytanic acid stores in brown adipose tissue thus suggesting that a high local exposure to phytanic acid in brown fat may contribute to signalling adaptive changes in the tissue in response to thermogenic activation. ß

show abstract

Section: Methodsmentioning

confidence: 99%

Phytanic acid, but not pristanic acid, mediates the positive effects of phytol derivatives on brown adipocyte differentiation

et al. 2002

Self Cite

View full text Add to dashboard Cite

show abstract

“…Transcriptional regulation of genes encoding enzymes such as SCD1, ACC1, and FAS is complex, and the direct targets for RIP140 action have yet to be elucidated. In BAT, transcription from the UCP1 gene may be regulated by PPARs, retinoids, and thyroid hormone, as well as through the activation of ␤-adrenergic receptor intracellular signaling pathways (19,(48)(49)(50)(51). Expression of UCP1 has been shown to be induced in WAT in transgenic mice by introduction of an activated form of PPAR␦ (20) and also in human white adipocytes in culture as a result of expression of PGC-1␣ and activation by ligands for PPAR␥ (52).…”

Section: Discussionmentioning

confidence: 99%

Nuclear receptor corepressor RIP140 regulates fat accumulation

Leonardsson

Steel

Christian

et al. 2004

Proc. Natl. Acad. Sci. U.S.A.

335

355

View full text Add to dashboard Cite

Nuclear receptors and their coactivators have been shown to function as key regulators of adipose tissue biology. Here we show that a ligand-dependent transcriptional repressor for nuclear receptors plays a crucial role in regulating the balance between energy storage and energy expenditure. Mice devoid of the corepressor protein RIP140 are lean, show resistance to high-fat diet-induced obesity and hepatic steatosis, and have increased oxygen consumption. Although the process of adipogenesis is unaffected, expression of certain lipogenic enzymes is reduced. In contrast, genes involved in energy dissipation and mitochondrial uncoupling, including uncoupling protein 1, are markedly increased. Therefore, the maintenance of energy homeostasis requires the action of a transcriptional repressor in white adipose tissue, and ligand-dependent recruitment of RIP140 to nuclear receptors may provide a therapeutic target in the treatment of obesity and related disorders. E nergy homeostasis is a highly regulated process that requires precise control of food intake and energy expenditure (1). The major and most efficient storage of energy occurs in the form of triglycerides in white adipose tissue (WAT), and it is now clear that the adipocyte itself may act as an endocrine cell such that altered adipocyte function would cause changes in systemic energy balance (2, 3). From adipogenic stores, fatty acids are easily mobilized during periods of energy restriction or increased physical activity to provide enough fuel for energy synthesis in the form of ATP. In addition, energy is dissipated by generating heat in brown adipose tissue (BAT) and skeletal muscles by regulating the uncoupling of ATP production from respiration. Many of these metabolic processes are controlled in part by nuclear receptors (4, 5), including peroxisome proliferatoractivated receptors (PPARs) (6, 7), thyroid hormone receptor (8, 9), estrogen receptor ␣ (ER␣) (10, 11), and ER-related receptor ␣ (ERR␣) (12). The best characterized of these are the PPARs, with PPAR␥ and PPAR␣ playing an essential role in adipogenesis (13-16) and in thermogenesis and fatty acid oxidation (17-19), respectively, whereas recent studies have implicated a role for PPAR␦ in lipid homeostasis (20).Nuclear receptors stimulate target gene transcription by recruiting coactivators that are required to remodel chromatin and facilitate the assembly of the basal transcription machinery (21). The key coactivator in metabolic processes is the PPAR␥ coactivator 1␣ (PGC-1␣) (22-25), which was initially shown to promote adaptive thermogenesis in BAT and which has emerged as a target for integrating signals in the regulation of specific metabolic programs in other tissues, including muscle and liver. More recently, the related coactivator PGC-1␤ (26, 27) has been implicated in the regulation of energy expenditure as a potential coactivator for ERR␣ (28). In addition, the p160 family of coactivators has also been found to control energy balance in adipose tissue. For instance, SRC1, in associatio...

show abstract

“…The genomic organization of the mouse, rat and human UCP1 genes has been analysed in several laboratories [7,8,[130][131][132][133][134][135][136][137][138][139][140][141][142][143][144][145]. The structure of the UCP1 gene is highly conserved in these three species.…”

Section: Genetics Of Ucpsmentioning

confidence: 99%

“…The response elements for these factors were functionally identified in the enhancer [132,[136][137][138][139][140][141]159]. Response elements for retinoids seem to be particularly important for the control of UCP1 gene transcription.…”

Section: Functional Dissection Of the Ucp1 Genementioning

confidence: 99%

The uncoupling protein homologues: UCP1, UCP2, UCP3, StUCP and AtUCP

Ricquier¹,

Bouillaud

2000

Biochemical Journal

607

115

View full text Add to dashboard Cite

Animal and plant uncoupling protein (UCP) homologues form a subfamily of mitochondrial carriers that are evolutionarily related and possibly derived from a proton\anion transporter ancestor. The brown adipose tissue (BAT) UCP1 has a marked and strongly regulated uncoupling activity, essential to the maintenance of body temperature in small mammals. UCP homologues identified in plants are induced in a cold environment and may be involved in resistance to chilling. The biochemical activities and biological functions of the recently identified mammalian UCP2 and UCP3 are not well known. However, recent data support a role for these UCPs in State 4 respiration, respiration uncoupling and proton leaks in mitochondria. Moreover, genetic studies suggest that UCP2 and UCP3 play a part in

show abstract

A Novel Regulatory Pathway of Brown Fat Thermogenesis

Cited by 182 publications

References 50 publications

Phytanic acid, but not pristanic acid, mediates the positive effects of phytol derivatives on brown adipocyte differentiation

Phytanic acid, but not pristanic acid, mediates the positive effects of phytol derivatives on brown adipocyte differentiation

Nuclear receptor corepressor RIP140 regulates fat accumulation

The uncoupling protein homologues: UCP1, UCP2, UCP3, StUCP and AtUCP

Contact Info

Product

Resources

About