Enhanced hepatitis C virus genome replication and lipid accumulation mediated by inhibition of AMP-activated protein kinase

Mankouri, Jamel; Tedbury, Philip R.; Gretton, Sarah N.; Hughes, Mair; Griffin, Stephen; Dallas, Mark L.; Green, Kevin A.; Hardie, D. Grahame; Peers, Chris; Harris, Mark

doi:10.1073/pnas.0912426107

Cited by 129 publications

(152 citation statements)

References 41 publications

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“…Thus, inhibition of AMPK by HCV would favor a reduction in fatty acid oxidation and thus an increase in hepatic lipid accumulation. 89 In contrast, Diamond and co-workers reported a sustained increase in fatty acid oxidation upon HCV infection, but also a stimulation of lipid biosynthesis. Although the significance of this simultaneous induction in lipid anabolism and catabolism remains unclear, the authors argue that β-oxidation may help to maintain elevated ATP levels to support energy-dependent biosynthetic processes as well as to limit the accumulation and toxic effect of ceramide overload.…”

Section: Role Of Lipid Metabolism In Hcv Rna Replicationmentioning

confidence: 94%

“…Indeed, recent studies based on transcriptome and proteomic analyses have demonstrated that expression of host genes involved in the biosynthesis, degradation and transport of intracellular lipids is profoundly altered upon infection. [86][87][88][89] The expression of SREBPs, which control transcription of genes required for cholesterol biosynthesis, 90 is stimulated both by HCV infection and It was demonstrated that NS proteins associate with cholesterol-rich lipid rafts and that depletion of cholesterol with statins selectively reduces HCV RNA replication. 104 However, statins are inhibitors of the mevalonate pathway, 99 which produces not only cholesterol, but also non-sterol isoprenoids, including geranylgeranyl and farnesyl.…”

Section: Role Of Lipid Metabolism In Hcv Rna Replicationmentioning

confidence: 99%

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Hepatitis c virus and host cell lipids: An intimate connection

Alvisi¹,

Madan²,

2011

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Section: Role Of Lipid Metabolism In Hcv Rna Replicationmentioning

confidence: 94%

Section: Role Of Lipid Metabolism In Hcv Rna Replicationmentioning

confidence: 99%

Hepatitis c virus and host cell lipids: An intimate connection

Alvisi¹,

Madan²,

2011

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“…In both cases, the biosynthetic machinery of the cell has been usurped by abnormal genes, by viral genes in the former case, and by oncogenic mutations or loss of tumor suppressors in the latter. The effects of viral infection on AMPK were recently studied using an in vitro model system in which a human hepatoma cell line was infected using hepatitis C virus (HCV) (Mankouri et al 2010). When HCV infects host cells it switches on both protein synthesis (making a single polyprotein that is cleaved into the 10 proteins encoded by the viral RNA genome) and fatty acid/triglyceride synthesis, which are required for the viral lipid envelope.…”

Section: Roles Of Ampk In Cancer and In Viral Infectionmentioning

confidence: 99%

“…When HCV infects host cells it switches on both protein synthesis (making a single polyprotein that is cleaved into the 10 proteins encoded by the viral RNA genome) and fatty acid/triglyceride synthesis, which are required for the viral lipid envelope. One might expect that the large increase in demand for ATP caused by rapid protein and lipid synthesis would lead to activation of AMPK, but in fact the opposite occurs, in that phosphorylation of Thr172 on AMPK is reduced relative to uninfected controls (Mankouri et al 2010). The mechanism responsible appears to be that one of the viral proteins (NS5A) binds to and activates phosphatidylinositol (PI) 3-kinase, leading to activation of the phosphatidylinositol trisphosphate (PIP 3 ) -activated kinase PKB/Akt (Street et al 2004).…”

Section: Roles Of Ampk In Cancer and In Viral Infectionmentioning

confidence: 99%

Adenosine Monophosphate-Activated Protein Kinase: A Central Regulator of Metabolism with Roles in Diabetes, Cancer, and Viral Infection

Hardie¹

2011

Cold Spring Harbor Symposia on Quantitative Biology

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Adenosine monophosphate -activated protein kinase (AMPK) is a cellular energy sensor activated by metabolic stresses that inhibit catabolic ATP production or accelerate ATP consumption. Once activated, AMPK switches on catabolic pathways, generating ATP, while inhibiting cell growth and proliferation, thus promoting energy homeostasis. AMPK is activated by the antidiabetic drug metformin, and by many natural products including "nutraceuticals" and compounds used in traditional medicines. Most of these xenobiotics activate AMPK by inhibiting mitochondrial ATP production. AMPK activation by metabolic stress requires the upstream kinase, LKB1, whose tumor suppressor effects may be largely mediated by AMPK. However, many tumor cells appear to have developed mechanisms to reduce AMPK activation and thus escape its growthrestraining effects. A similar phenomenon occurs during viral infection. If we can establish how down-regulation occurs in tumors and virus-infected cells, there may be therapeutic avenues to reverse these effects.

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“…It is intriguing, however, that separate research has shown that experimental hepatitis C infection is associated with downregulation of AMPK activity, and that restoring AMPK activation by metformininduced energy stress reduces viral infection and some of its consequences (16). Another example of interesting research in this context is evidence that insulin (which reaches the liver in high concentrations in the hyperinsulinemic phase of type II diabetes) is sufficient to induce liver cancer (17,18); thus, information concerning insulin levels and signaling downstream of the insulin receptor in the presence and absence of metformin in the model of Bhalla and colleagues (2) would be of interest.…”

mentioning

confidence: 99%

Metformin and Hepatic Carcinogenesis

Pollak

González-Angulo

2012

Cancer Prevention Research

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Retrospective, hypothesis-generating population studies suggest that diabetics treated with metformin have a substantially reduced risk of several cancers, including hepatoma, relative to diabetics on other therapies. In this issue of the journal (beginning on page 544), Bhalla and colleagues contribute to the growing literature on metformin effects in experimental carcinogenesis models, showing reduced carcinogen-induced hepatoma in mice. The clinical need to develop novel prevention strategies for hepatoma is obvious, given an increasing prevalence and poor prognosis. The clues that metformin or related biguanides may have utility in this area justify accelerated laboratory research, as more data concerning mechanism, pharmacokinetics, and predictors of efficacy will help to optimize the design of clinical trials. Cancer Prev Res; 5(4); 500-2. Ó2012 AACR.The literature on metformin and cancer has grown rapidly in the past few years. There is tantalizing evidence that this widely used, well-tolerated biguanide molecule may have applications in cancer prevention or treatment (1). In this issue of the journal, Bhalla and colleagues present interesting experimental evidence for an action of metformin in inhibiting the development of chemically induced hepatocellular carcinoma in mice (2), yet many important questions remain unanswered.Several proposed mechanisms of action of metformin may underlie its activity as a cancer preventive agent. Some (but not all) of these mechanisms may overlap with the actions that are responsible for the utility of the compound in the treatment of type II diabetes. It is now thought that the pleiotropic effects of metformin originate with the primary actions of the drug on the mitochondria (3), where it inhibits oxidative phosphorylation (at respiratory complex I) in a manner that has not yet been described in detail. Sequelae to this inhibition occur at the local mitochondrial level, at the cellular level, and at the level of the whole organism. The best known local consequence is the decline of mitochondrial ATP production (1), but there is also recent evidence for altered redox status, a decrease in reactive oxygen species (ROS) production, and a decrease in mutations attributable to ROS (4). At the cellular level, the reduction in ATP production by oxidative phosphorylation leads to a degree of energy stress. This stress can have different effects depending on the cellular context. Some cells have the ability to sense and respond to the stress by decreasing energy-consuming processes such as lipid synthesis, protein synthesis, and proliferation (1, 3). This decrease results in a new steady state characterized by reduced ATP production, reduced ATP consumption, and an energetically "sleepy" phenotype, which may tend to slow carcinogenesis and may also be cytostatic for a subset of established cancers. Another compensation involves increasing glycolysis to help correct the ATP deficit. This process may seem paradoxical at first, as it represents a situation of increased glu...

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Enhanced hepatitis C virus genome replication and lipid accumulation mediated by inhibition of AMP-activated protein kinase

Cited by 129 publications

References 41 publications

Hepatitis c virus and host cell lipids: An intimate connection

Hepatitis c virus and host cell lipids: An intimate connection

Adenosine Monophosphate-Activated Protein Kinase: A Central Regulator of Metabolism with Roles in Diabetes, Cancer, and Viral Infection

Metformin and Hepatic Carcinogenesis

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