Histone Deacetylase 1 (HDAC1) Negatively Regulates Thermogenic Program in Brown Adipocytes via Coordinated Regulation of Histone H3 Lysine 27 (H3K27) Deacetylation and Methylation

Li, Fenfen; Wu, Rui; Cui, Xin; Zha, Lin; Yu, Liqing; Shi, Hang; Xue, Bingzhong

doi:10.1074/jbc.m115.677930

Cited by 93 publications

(109 citation statements)

References 65 publications

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“…Adipose-selective transgenic expression of FOXC2 increases intracellular cAMP levels by increasing the expression of PKA (the RIα subunit) and promotes beige adipocyte thermogenesis in WAT 62 . By contrast, histone deacetylase HDAC1 (and HDAC2) inhibits thermogenesis through deacetylation of H3K27 on the regulatory regions of Ucp1 , which then inhibits CREB and ATF2 mediated transcription 74 . Intriguingly it has been recently found that casein kinase 2 (CK2) activity in response to β-AR signalling is preferentially increased in WAT and inhibits the thermogenic programme in this tissue.…”

Section: Regulation Of Adipocyte Thermogenesismentioning

confidence: 99%

Transcriptional and epigenetic control of brown and beige adipose cell fate and function

Inagaki

Sakai

Kajimura

2016

Nat Rev Mol Cell Biol

269

267

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White adipocytes store excess energy in the form of triglycerides, whereas brown and beige adipocytes dissipate energy in the form of heat. This thermogenic function relies on the activation of brown and beige adipocyte-specific gene programmes that are coordinately regulated by adipose-selective chromatin architectures and by a set of unique transcriptional and epigenetic regulators. A number of transcriptional and epigenetic regulators are also required for promoting beige adipocyte biogenesis in response to various environmental stimuli. A better understanding of the molecular mechanisms governing the generation and function of brown and beige adipocytes is necessary to allow us to control adipose cell fate and stimulate thermogenesis. This may provide a therapeutic approach for the treatment of obesity and obesity-associated diseases, such as type 2 diabetes.

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Section: Regulation Of Adipocyte Thermogenesismentioning

confidence: 99%

Transcriptional and epigenetic control of brown and beige adipose cell fate and function

Inagaki

Sakai

Kajimura

2016

Nat Rev Mol Cell Biol

269

267

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“…LSD1 is recruited to brown/beige adipogenic enhancers through its interactions with transcription factors Nrf1 and Zfp516 (71, 267). Cold exposure decreases histone deacetylase 1 (Hdac1) levels in BAT, and β adrenergic signaling decreases the binding of Hdac1 to the UCP1 and PGC1α promoters in brown adipocytes, leading to an increase in active epigenetic H3K27ac mark (181). Concurrently, β adrenergic signaling stimulates dissociation of enhancer of zeste homologue (Ezh2) and suppressor of zeste 12 (SUZ12), leading to a decrease in repressive epigenetic mark H3K27me3 at the UCP1 and PGC1α promoters (181).…”

Section: Genetic and Epigenetic Regulation Of Brown And Beige Fat Thementioning

confidence: 99%

Brown and Beige Adipose Tissues in Health and Disease

Rui

2017

Comprehensive Physiology

143

113

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Brown and beige adipocytes arise from distinct developmental origins. Brown adipose tissue (BAT) develops embryonically from precursors that also give to skeletal muscle. Beige fat develops postnatally and is highly inducible. Beige fat recruitment is mediated by multiple mechanisms, including de novo beige adipogenesis and white-to-brown adipocyte transdifferentiaiton. Beige precursors reside around vasculatures, and proliferate and differentiate into beige adipocytes. PDGFRα+Ebf2+ precursors are restricted to beige lineage cells, while another PDGFRα+ subset gives rise to beige adipocytes, white adipocytes, or fibrogenic cells. White adipocytes can be reprogramed and transdifferentiated into beige adipocytes. Brown and beige adipocytes display many similar properties, including multilocular lipid droplets, dense mitochondria, and expression of UCP1. UCP1-mediated thermogenesis is a hallmark of brown/beige adipocytes, albeit UCP1-independent thermogenesis also occurs. Development, maintenance, and activation of BAT/beige fat are guided by genetic and epigenetic programs. Numerous transcriptional factors and coactivators act coordinately to promote BAT/beige fat thermogenesis. Epigenetic reprograming also influences expression of brown/beige adipocyte-selective genes. BAT/beige fat is regulated by neuronal, hormonal, and immune mechanisms. Hypothalamic thermal circuits define the temperature setpoint that guides BAT/beige fat activity. Metabolic hormones, paracrine/autocrine factors, and various immune cells also play a critical role in regulating BAT/beige fat functions. BAT and beige fat defend temperature homeostasis, and regulate body weight and glucose and lipid metabolism. Obesity is associated with brown/beige fat deficiency, and reactivation of brown/beige fat provides metabolic health benefits in some patients. Pharmacological activation of BAT/beige fat may hold promise for combating metabolic diseases.

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“…The favourable open chromatin structure for Ucp1 transcriptional activation after β-AR stimulation has been previously reported in cultured brown adipocyte, demonstrated by a significant increase of H3K27ac in both the Ucp1 and Pgc1α promoter regions [12]. However, which factors regulate behind this phenomenon is still unclear.…”

Section: Discussionmentioning

confidence: 93%

β-adrenergic Receptor Stimulation Revealed a Novel Regulatory Pathway via Suppressing Histone Deacetylase 3 to Induce Uncoupling Protein 1 Expression in Mice Beige Adipocyte

Yuliana

Jheng

Kawarasaki

et al. 2018

IJMS

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Browning of adipose tissue has been prescribed as a potential way to treat obesity, marked by the upregulation of uncoupling protein 1 (Ucp1). Several reports have suggested that histone deacetylase (HDAC) might regulate Ucp1 by remodelling chromatin structure, although the mechanism remains unclear. Herein, we investigate the effect of β-adrenergic receptor (β-AR) activation on the chromatin state of beige adipocyte. β-AR-stimulated Ucp1 expression via cold (in vivo) and isoproterenol (in vitro) resulted in acetylation of histone activation mark H3K27. H3K27 acetylation was also seen within Ucp1 promoter upon isoproterenol addition, favouring open chromatin for Ucp1 transcriptional activation. This result was found to be associated with the downregulation of class I HDAC mRNA, particularly Hdac3 and Hdac8. Further investigation showed that although HDAC8 activity decreased, Ucp1 expression was not altered when HDAC8 was activated or inhibited. In contrast, HDAC3 mRNA and protein levels were simultaneously downregulated upon isoproterenol addition, resulting in reduced recruitment of HDAC3 to the Ucp1 enhancer region, causing an increased H3K27 acetylation for Ucp1 upregulation. The importance of HDAC3 inhibition was confirmed through the enhanced Ucp1 expression when the cells were treated with HDAC3 inhibitor. This study highlights the novel mechanism of HDAC3-regulated Ucp1 expression during β-AR stimulation.

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Histone Deacetylase 1 (HDAC1) Negatively Regulates Thermogenic Program in Brown Adipocytes via Coordinated Regulation of Histone H3 Lysine 27 (H3K27) Deacetylation and Methylation

Cited by 93 publications

References 65 publications

Transcriptional and epigenetic control of brown and beige adipose cell fate and function

Transcriptional and epigenetic control of brown and beige adipose cell fate and function

Brown and Beige Adipose Tissues in Health and Disease

β-adrenergic Receptor Stimulation Revealed a Novel Regulatory Pathway via Suppressing Histone Deacetylase 3 to Induce Uncoupling Protein 1 Expression in Mice Beige Adipocyte

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