Akt Stimulates Hepatic SREBP1c and Lipogenesis through Parallel mTORC1-Dependent and Independent Pathways

Yecies, Jessica L.; Zhang, Hui H.; Menon, Suchithra; Liu, Sihao; Yecies, Derek; Lipovsky, Alex; Görgün, Cem Z.; Kwiatkowski, David J.; Hotamışlıgil, Gökhan S.; Lee, Chih‐Hao; Manning, Brendan D.

doi:10.1016/j.cmet.2011.06.002

Cited by 521 publications

(366 citation statements)

References 51 publications

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“…The increased mTORC1 activity in Grb14i mice can therefore be also driven by p62 in addition to insulin receptor stimulation, contributing to the positive feedback loop. After a nutritional challenge, insulin-dependent de novo fatty acid synthesis and liver lipid accumulation are mediated by the activation of SREBP-1c in an mTORC1-dependent manner (51,52). The observation that p62 is not phosphorylated by mTORC1 in liver of refed control mice is thus consistent with the activation of the lipogenic pathway in this situation.…”

Section: Discussionsupporting

confidence: 72%

Novel Grb14-Mediated Cross Talk between Insulin and p62/Nrf2 Pathways Regulates Liver Lipogenesis and Selective Insulin Resistance

Popineau

Morzyglod

Carré

et al. 2016

Molecular and Cellular Biology

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A long-standing paradox in the pathophysiology of metabolic diseases is the selective insulin resistance of the liver. It is characterized by a blunted action of insulin to reduce glucose production, contributing to hyperglycemia, while de novo lipogenesis remains insulin sensitive, participating in turn to hepatic steatosis onset. The underlying molecular bases of this conundrum are not yet fully understood. Here, we established a model of selective insulin resistance in mice by silencing an inhibitor of insulin receptor catalytic activity, the growth factor receptor binding protein 14 (Grb14) in liver. Indeed, Grb14 knockdown enhanced hepatic insulin signaling but also dramatically inhibited de novo fatty acid synthesis. In the liver of obese and insulin-resistant mice, downregulation of Grb14 markedly decreased blood glucose and improved liver steatosis. Mechanistic analyses showed that upon Grb14 knockdown, the release of p62/sqstm1, a partner of Grb14, activated the transcription factor nuclear factor erythroid-2-related factor 2 (Nrf2), which in turn repressed the lipogenic nuclear liver X receptor (LXR). Our study reveals that Grb14 acts as a new signaling node that regulates lipogenesis and modulates insulin sensitivity in the liver by acting at a crossroad between the insulin receptor and the p62-Nrf2-LXR signaling pathways.

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Section: Discussionsupporting

confidence: 72%

Novel Grb14-Mediated Cross Talk between Insulin and p62/Nrf2 Pathways Regulates Liver Lipogenesis and Selective Insulin Resistance

Popineau

Morzyglod

Carré

et al. 2016

Molecular and Cellular Biology

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“…Such mechanisms have been shown to be responsible for similar paradoxical findings upon disruption of the TSC complex in other cell types by affecting mTORC1‐independent targets of these pathways (Byles et al, 2013; Tang et al, 2014; Yecies et al, 2011) (Figure 4). Indeed, similar to other cell types, hyperactivation of mTORC1 after deletion of TSC1 or TSC2 suppressed Akt activity in both SCs and OLs (Beirowski et al, 2017; Figlia et al, 2017; Lebrun‐Julien et al, 2014).…”

Section: Myelination and Mtormentioning

confidence: 80%

Myelination and mTOR

Figlia

Gerber

Suter

2017

Glia

133

120

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Myelinating cells surround axons to accelerate the propagation of action potentials, to support axonal health, and to refine neural circuits. Myelination is metabolically demanding and, consistent with this notion, mTORC1—a signaling hub coordinating cell metabolism—has been implicated as a key signal for myelination. Here, we will discuss metabolic aspects of myelination, illustrate the main metabolic processes regulated by mTORC1, and review advances on the role of mTORC1 in myelination of the central nervous system and the peripheral nervous system. Recent progress has revealed a complex role of mTORC1 in myelinating cells that includes, besides positive regulation of myelin growth, additional critical functions in the stages preceding active myelination. Based on the available evidence, we will also highlight potential nonoverlapping roles between mTORC1 and its known main upstream pathways PI3K‐Akt, Mek‐Erk1/2, and AMPK in myelinating cells. Finally, we will discuss signals that are already known or hypothesized to be responsible for the regulation of mTORC1 activity in myelinating cells.

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“…[9][10][11]35 The result is a measureable increase in rates of lipid synthesis within 6 hours of mTORC1 activation; for instance, as observed in primary hepatocytes stimulated with insulin. 34 As described above, the activation of SREBP also leads to the transcriptional activation of NRF1, resulting in a substantial increase in its abundance in cells and tissue by 6 hours.…”

Section: Temporal Influence Of Mtorc1 Signaling On Protein Homeostasismentioning

confidence: 99%

“…33 It has become clear that the SREBPs are a major transcriptional effector of mTORC1 signaling in multiple cellular settings. [9][10][11]34,35 Lipids serve as a major source of stored energy that can be mobilized quickly, and growing cells have an increased demand for lipids for the production of new membranes. mTORC1 plays a central role in the control of cell growth, and evidence indicate that the activation of SREBPdependent lipid synthesis is one essential downstream factor in its promotion of growth.…”

Section: Nrf1 and Its Physiological Activation By Mtorc1 And Srebp1mentioning

confidence: 99%

mTORC1 signaling activates NRF1 to increase cellular proteasome levels

Zhang

Manning

2015

Cell Cycle

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Akt Stimulates Hepatic SREBP1c and Lipogenesis through Parallel mTORC1-Dependent and Independent Pathways

Cited by 521 publications

References 51 publications

Novel Grb14-Mediated Cross Talk between Insulin and p62/Nrf2 Pathways Regulates Liver Lipogenesis and Selective Insulin Resistance

Novel Grb14-Mediated Cross Talk between Insulin and p62/Nrf2 Pathways Regulates Liver Lipogenesis and Selective Insulin Resistance

Myelination and mTOR

mTORC1 signaling activates NRF1 to increase cellular proteasome levels

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