ER Stress Inhibits Liver Fatty Acid Oxidation while Unmitigated Stress Leads to Anorexia-Induced Lipolysis and Both Liver and Kidney Steatosis

DeZwaan-McCabe, Diane; Sheldon, Ryan D.; Gorecki, Michelle C.; Guo, Deng‐Fu; Gansemer, Erica R.; Kaufman, Randal J.; Rahmouni, Kamal; Gillum, Matthew P.; Taylor, Eric B.; Teesch, Lynn M.; Rutkowski, D. Thomas

doi:10.1016/j.celrep.2017.05.020

Cited by 80 publications

(63 citation statements)

References 47 publications

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“…ER stress also resulted in upregulation of FGF21 via ATF4 and, as a result, increased serum FGF21 . We showed that pharmacological ER stress also inhibits hepatic fatty acid oxidation; this is likely due to genetic suppression of genes that regulate the process . This suppression is partially due to the action of CHOP.…”

Section: Regulation Of Metabolism By Hepatic Er Stressmentioning

confidence: 72%

“…Although obesity elicits ER stress, it might be that overnutrition per se —i.e., taking in too many calories—causes or exacerbates hepatic ER stress independent of the associated obesity. The simple act of eating a meal after a prolonged fast is sufficient to activate the UPR in the liver in mice . This finding suggests that feeding itself perturbs hepatic ER function, though presumably this perturbation and its downstream consequences are transient.…”

Section: Pathways From Obesity To Er Stressmentioning

confidence: 99%

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Liver function and dysfunction – a unique window into the physiological reach of ER stress and the unfolded protein response

Rutkowski

2018

The FEBS Journal

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The unfolded protein response (UPR) improves endoplasmic reticulum (ER) protein folding in order to alleviate stress. Yet it is becoming increasingly clear that the UPR regulates processes well beyond those directly involved in protein folding, in some cases by mechanisms that fall outside the realm of canonical UPR signaling. These pathways are highly specific from one cell type to another, implying that ER stress signaling affects each tissue in a unique way. Perhaps nowhere is this more evident than in the liver, which-beyond being a highly secretory tissue-is a key regulator of peripheral metabolism and a uniquely proliferative organ upon damage. The liver provides a powerful model system for exploring how and why the UPR extends its reach into physiological processes that occur outside the ER, and how ER stress contributes to the many systemic diseases that involve liver dysfunction. This review will highlight the ways in which the study of ER stress in the liver has expanded the view of the UPR to a response that is a key guardian of cellular homeostasis outside of just the narrow realm of ER protein folding.

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Section: Regulation Of Metabolism By Hepatic Er Stressmentioning

confidence: 72%

Section: Pathways From Obesity To Er Stressmentioning

confidence: 99%

Liver function and dysfunction – a unique window into the physiological reach of ER stress and the unfolded protein response

Rutkowski

2018

The FEBS Journal

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“…Lipid accumulation in a tissue is dependent not only on lipogenesis but also on other mechanisms, such as increased lipid deposition, decreased lipolysis and/or reduced triglyceride output (Cohen et al 2011). Tunicamycin affects several pathways contributing to the hepatic lipid accumulation, including inhibition of fatty acid oxidation (DeZwaan-McCabe et al 2017), upregulation of the very low-density lipoprotein receptor (Jo et al 2013) and inhibition of efflux of triglyceride (Qiu et al 2006, Ota et al 2008. Interestingly, while tunicamycin inhibits the mRNA expression of lipogenic genes such as Fas and Srebf1 in liver (Rutkowski et al 2008), tunicamycin treatment for either 8 h or 24 h had no significant effect on lipogenic activity (DeZwaan-McCabe et al 2017).…”

Section: Discussionmentioning

confidence: 99%

De-silencing Grb10 contributes to acute ER stress-induced steatosis in mouse liver

Luo

Jiang

Liu

et al. 2018

Journal of Molecular Endocrinology

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The growth factor receptor bound protein GRB10 is an imprinted gene product and a key negative regulator of the insulin, IGF1 and mTORC1 signaling pathways. GRB10 is highly expressed in mouse fetal liver but almost completely silenced in adult mice, suggesting a potential detrimental role of this protein in adult liver function. Here we show that the gene could be reactivated in adult mouse liver by acute endoplasmic reticulum stress (ER stress) such as tunicamycin or a short-term high-fat diet (HFD) challenge, concurrently with increased unfolded protein response (UPR) and hepatosteatosis. Lipogenic gene expression and acute ER stress-induced hepatosteatosis were significantly suppressed in the liver of the liver-specific GRB10 knockout mice, uncovering a key role of reactivation in acute ER stress-induced hepatic lipid dysregulation. Mechanically, acute ER stress induces reactivation via an ATF4-mediated increase in gene transcription. Our study demonstrates for the first time that the silenced gene can be reactivated by acute ER stress and its reactivation plays an important role in the early development of hepatic steatosis.

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“…76,77 Conversely, more recent studies have challenged whether ER stress promotes hepatic lipogenesis. 67,[78][79][80] It has been argued that ER stress may, in fact, suppress hepatic lipogenesis. [78][79][80] In comparing the various studies exploring this issue, it is important to bear in mind that the effects of ER stress are extremely dependent on the experimental conditions employed.…”

Section: De Novo Lipogenesismentioning

confidence: 99%

“…67,[78][79][80] It has been argued that ER stress may, in fact, suppress hepatic lipogenesis. [78][79][80] In comparing the various studies exploring this issue, it is important to bear in mind that the effects of ER stress are extremely dependent on the experimental conditions employed. Moreover, the UPR is a highly dynamic signaling cascade that can have variable, and even opposing, outcomes depending on the degree and duration of ER stress.…”

Section: De Novo Lipogenesismentioning

confidence: 99%

Unfolded Protein Response Sensors in Hepatic Lipid Metabolism and Nonalcoholic Fatty Liver Disease

Henkel

2018

Semin Liver Dis

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Activation of the hepatic unfolded protein response (UPR), a highly conserved cellular response to endoplasmic reticulum (ER) stress, is a firmly established feature of nonalcoholic fatty liver disease (NAFLD). ER stress is now widely accepted as both a cause and a consequence of hepatic steatosis. Moreover, the accumulation of hepatic lipids induces ER stress, which, in turn, disrupts hepatic lipid metabolism thus creating a vicious cycle that potentiates hepatic lipid accumulation. Additionally, there is interplay between the UPR and the inflammatory cascades associated with progressive nonalcoholic steatohepatitis. Understanding the molecular mechanisms by which the UPR regulates hepatic lipid metabolism and lipotoxic liver injury may lead to the identification of novel therapeutic targets for the treatment of NAFLD.

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ER Stress Inhibits Liver Fatty Acid Oxidation while Unmitigated Stress Leads to Anorexia-Induced Lipolysis and Both Liver and Kidney Steatosis

Cited by 80 publications

References 47 publications

Liver function and dysfunction – a unique window into the physiological reach of ER stress and the unfolded protein response

Liver function and dysfunction – a unique window into the physiological reach of ER stress and the unfolded protein response

De-silencing Grb10 contributes to acute ER stress-induced steatosis in mouse liver

Unfolded Protein Response Sensors in Hepatic Lipid Metabolism and Nonalcoholic Fatty Liver Disease

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