Downregulation of AMP-activated protein kinase by Cidea-mediated ubiquitination and degradation in brown adipose tissue

Qi, Jingzong; Gong, Jingyi; Zhao, Tong‐Jin; Zhao, Jie; Lam, Pui-ying; Ye, Jing; Li, John; Wu, Jiawei; Zhou, Hai; Li, Peng

doi:10.1038/emboj.2008.92

Cited by 141 publications

(133 citation statements)

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“…Studies to date indicate that protein-protein interactions are important to CIDE protein function, and both CIDEA and CIDEB have been studied somewhat in this regard. Homo-and heterodimeric interaction of CIDEA and/or CIDEB (i.e., CIDEA:CIDEA, CIDEB:CIDEB, and CIDEA:CIDEB) has been reported (5,8,11,19,27). CIDEB interacts with viral protein NS2 (8) and apolipoprotein B (42) and CIDEA with AMPK (27); such interactions appear to impact the physiological function of these CIDE partner proteins.…”

Section: Ajp-endocrinol Metabmentioning

confidence: 99%

“…Ectopic expression of an HA-tagged or eGFP fusion construct containing amino acids 166 -195 of CIDEB was sufficient for lipid droplet targeting in lipid-loaded COS cells and HepG2 hepatocytes, respectively (42). CIDEA and CIDEB are also reportedly localized to the endoplasmic reticulum, an organelle from which biogenesis of intracellular lipid droplets initiates (27,42). Moreover, in addition to being lipid droplet-localized proteins per se, ectopic expression of FSP27 and CIDEA has been demonstrated to promote the formation and/or enlargement of lipid droplets in several nonadipocyte cell types, a phenomenon that is particularly evident with addition of exogenous oleic acid to culture media.…”

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confidence: 99%

“…CIDEA-null mice exhibit elevated lipolysis in BAT and resist diet-induced obesity (44). A recent report demonstrated that one mechanism of CIDEA action is via its interaction with the major metabolic regulator AMP-activated protein kinase (AMPK), which reduces AMPK protein level by enhancing proteosome-mediated AMPK degradation (27). The phenotype of CIDEA-null mice was attributed initially to the ability of CIDEA to regulate thermogenesis via interaction with uncoupling protein-1 (UCP1) to inhibit UCP1 activity (44).…”

mentioning

confidence: 99%

“…The phenotype of CIDEA-null mice was attributed initially to the ability of CIDEA to regulate thermogenesis via interaction with uncoupling protein-1 (UCP1) to inhibit UCP1 activity (44). Given that the initial mitochondrial localization reported for CIDEA appears to not be the case (27), CIDEA interaction with UCP1 remains to be fully clarified. CIDEB interacts with apolipoprotein B and promotes the formation of triacylglycerol-enriched VLDL particles (42).…”

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confidence: 99%

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Functional analysis of FSP27 protein regions for lipid droplet localization, caspase-dependent apoptosis, and dimerization with CIDEA

Liu

Zhou

Kim

et al. 2009

American Journal of Physiology-Endocrinology and Metabolism

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MS, Smas CM.Functional analysis of FSP27 protein regions for lipid droplet localization, caspase-dependent apoptosis, and dimerization with CIDEA. Am J Physiol Endocrinol Metab 297: E1395-E1413, 2009. First published October 20, 2009 doi:10.1152/ajpendo.00188.2009.-The adipocytespecific protein FSP27, also known as CIDEC, is one of three cell death-inducing DFF45-like effector (CIDE) proteins. The first known function for CIDEs was promotion of apoptosis upon ectopic expression in mammalian cells. Recent studies in endogenous settings demonstrated key roles for CIDEs in energy metabolism. FSP27 is a lipid droplet-associated protein whose heterologous expression enhances formation of enlarged lipid droplets and is required for unilocular lipid droplets typical of white adipocytes in vivo. Here, we delineate relationships between apoptotic function and lipid droplet localization of FSP27. We demonstrate that ectopic expression of FSP27 induces enlarged lipid droplets in multiple human cell lines, which is indicative that its mechanism involves ubiquitously present, rather than adipocyte-specific, cellular machinery. Furthermore, promotion of lipid droplet formation in HeLa cells via culture in exogenous oleic acid offsets FSP27-mediated apoptosis. Using transient cotransfections and analysis of lipid droplets in HeLa cells stably expressing FSP27, we show that FSP27 does not protect lipid droplets from action of ATGL lipase. Domain mapping with eGFP-FSP27 deletion constructs indicates that lipid droplet localization of FSP27 requires amino acids 174 -192 of its CIDE C domain. The apoptotic mechanism of FSP27, which we show involves caspase-9 and mitochondrial cytochrome c, also requires this 19-amino acid region. Interaction assays determine the FSP27 CIDE C domain complexes with CIDEA, and Western blot reveals that FSP27 protein levels are reduced by coexpression of CIDEA. Overall, our findings demonstrate the function of the FSP27 CIDE C domain and/or regions thereof for apoptosis, lipid droplet localization, and CIDEA interaction.fat-specific protein 27; cell death-inducing DFF45-like effector A; adipose OBESITY AND ITS RELATED COMORBIDITIES are approaching epidemic levels (1, 9). The development of new therapeutic inroads to treat these conditions would be greatly facilitated by a full understanding of lipid homeostasis (35,36). Lipotoxicity is a highly detrimental outcome of the obese state, leading to derangement of cell function and/or cell death in various tissues (34,35,37). White adipocytes present in white adipose tissue are the major site storage of excess energy in the form of triacylglycerol, contained within intracellular lipid droplets (7,38). Efficient storage of excess fatty acids within adipocyte lipid droplets also serves to protect other cells and tissues from their lipotoxic effects (7, 38). Lipid droplets are highly dynamic organelles consisting of a neutral lipid core, a phospholipid monolayer, and a large number of lipid droplet-associated proteins (7, 38). The role for the vast majority ...

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Section: Ajp-endocrinol Metabmentioning

confidence: 99%

mentioning

confidence: 99%

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confidence: 99%

mentioning

confidence: 99%

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Functional analysis of FSP27 protein regions for lipid droplet localization, caspase-dependent apoptosis, and dimerization with CIDEA

Liu

Zhou

Kim

et al. 2009

American Journal of Physiology-Endocrinology and Metabolism

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“…, independent of AMP (Hardie 2008;McGee and Hargreaves 2010). As described in BAT (Qi et al 2008), AMPK is negatively regulated by cell-deathinducing like effector A (Cidea), inducing ubiquitination of the b subunit of AMPK and degradation of the enzyme. Also protein kinase A-mediated phosphorylation of a1-AMPK subunit at Ser-173 prevents activation of AMPK by LKB1-mediated phosphorylation of the a1-AMPK subunit at Thr-172, as found recently in white adipocytes (Djouder et al 2010).…”

Section: Role Of Ampk In Energy Metabolism and Glucose Homeostasismentioning

confidence: 99%

Augmenting energy expenditure by mitochondrial uncoupling: a role of AMP-activated protein kinase

et al. 2011

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Strategies to prevent and treat obesity aim to decrease energy intake and/or increase energy expenditure. Regarding the increase of energy expenditure, two key intracellular targets may be considered (1) mitochondrial oxidative phosphorylation, the major site of ATP production, and (2) AMP-activated protein kinase (AMPK), the master regulator of cellular energy homeostasis. Experiments performed mainly in transgenic mice revealed a possibility to ameliorate obesity and associated disorders by mitochondrial uncoupling in metabolically relevant tissues, especially in white adipose tissue (WAT), skeletal muscle (SM), and liver. Thus, ectopic expression of brown fat-specific mitochondrial uncoupling protein 1 (UCP1) elicited major metabolic effects both at the cellular/tissue level and at the whole-body level. In addition to expected increases in energy expenditure, surprisingly complex phenotypic effects were detected. The consequences of mitochondrial uncoupling in WAT and SM are not identical, showing robust and stable obesity resistance accompanied by improvement of lipid metabolism in the case of ectopic UCP1 in WAT, while preservation of insulin sensitivity in the context of high-fat feeding represents the major outcome of muscle UCP1 expression. These complex responses could be largely explained by tissue-specific activation of AMPK, triggered by a depression of cellular energy charge. Experimental data support the idea that (1) while being always activated in response to mitochondrial uncoupling and compromised intracellular energy status in general, AMPK could augment energy expenditure and mediate local as well as whole-body effects; and (2) activation of AMPK alone does not lead to induction of energy expenditure and weight reduction.

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Profilin upregulation induces autophagy through stabilization of AMP‐activated protein kinase

Saurav

Manna

2022

FEBS Letters

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Profilin regulates actin polymerization, and its balanced expression is required for cellular growth and development. Most tumours have compromised profilin expression, and its overexpression in MDA MB-231 breast cancer cells has been reported to activate AMP-activated protein kinase a (AMPKa), an energy-sensing molecule that affects various cellular processes including autophagy. This study aims to explore the role of profilin in autophagy induction. We employed all-trans retinoic acid (ATRA) as an inducer of profilin expression and showed that profilin induces autophagy through mTOR inhibition, autophagy-activating kinase ULK1 upregulation, and AMPK stabilization as well as its activation. Furthermore, evidence from our study indicates physical interaction between profilin and AMPK, which results in AMPK stabilization and induction of prolonged autophagy, thereby leading to apoptosis. This study uncovers a novel mechanism that induces autophagy in triple-negative breast cancer cells.

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Downregulation of AMP-activated protein kinase by Cidea-mediated ubiquitination and degradation in brown adipose tissue

Cited by 141 publications

References 51 publications

Functional analysis of FSP27 protein regions for lipid droplet localization, caspase-dependent apoptosis, and dimerization with CIDEA

Functional analysis of FSP27 protein regions for lipid droplet localization, caspase-dependent apoptosis, and dimerization with CIDEA

Augmenting energy expenditure by mitochondrial uncoupling: a role of AMP-activated protein kinase

Profilin upregulation induces autophagy through stabilization of AMP‐activated protein kinase

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