p53 and TIGAR regulate cardiac myocyte energy homeostasis under hypoxic stress

Kimata, Masaki; Matoba, Satoaki; Iwai-Kanai, Eri; Nakamura, Hideo; Hoshino, Atsushi; Nakaoka, Mikihiko; Katamura, Maki; Okawa, Yoshifumi; Mita, Yuichiro; Okigaki, Mitsuhiko; Ikeda, Koji; Tatsumi, Tomohide; Matsubara, Hiroaki

doi:10.1152/ajpheart.00250.2010

Cited by 64 publications

(61 citation statements)

References 39 publications

(46 reference statements)

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“…Because TIGAR cannot localize to the mitochondria in the absence of HIF1α, these results support the suggestion that mitochondrial localization and HK2 binding are important for the survival function of TIGAR in response to hypoxia. Discussion TIGAR has been shown to function as a Fru-2,6-BPase, regulating intracellular Fru-2,6-BP levels and glycolysis under various conditions (16,17,21,23). In this study, we identified an additional function for TIGAR in lowering ROS and maintaining cell survival during hypoxia through a mechanism that is independent of Fru-2,6-BPase activity.…”

Section: Resultsmentioning

confidence: 65%

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Mitochondrial localization of TIGAR under hypoxia stimulates HK2 and lowers ROS and cell death

Cheung

Ludwig

Vousden

2012

Proc. Natl. Acad. Sci. U.S.A.

207

168

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The p53-inducible protein TIGAR (Tp53-induced Glycolysis and Apoptosis Regulator) functions as a fructose-2,6-bisphosphatase (Fru-2,6-BPase), and through promotion of the pentose phosphate pathway, increases NADPH production to help limit reactive oxygen species (ROS). Here, we show that under hypoxia, a fraction of TIGAR protein relocalized to mitochondria and formed a complex with hexokinase 2 (HK2), resulting in an increase in HK2 activity. Mitochondrial localization of TIGAR depended on mitochondrial HK2 and hypoxia-inducible factor 1 (HIF1α) activity. The ability of TIGAR to function as a Fru-2,6-BPase was independent of HK2 binding and mitochondrial localization, although both of these activities can contribute to the full activity of TIGAR in limiting mitochondrial ROS levels and protecting from cell death.cancer metabolism | glycolysis | oxidative stress | low oxygen T he uptake and metabolism of glucose is fundamental for energy production and supporting various anabolic pathways that produce the macromolecules required for cell growth and proliferation. Flux through the different metabolic pathways can be modulated in response to varying growth conditions and demands, as seen in cancer cells, which adopt high rates of aerobic glycolysis that is characterized by extensive glucose uptake and high levels of lactate production (1).Glycolysis can be regulated by changes in the expression or activity of enzymes that catalyze various steps of the pathways. Allosteric regulation or covalent modification of many metabolic enzymes has been described, and the concentration of the active enzyme can also be controlled through changes in transcription, splicing, or protein stability. The subcellular localization of some glycolytic enzymes has also been shown to play an important role in regulating their functions (2, 3). In the first step of glucose metabolism, hexokinases (HK) generate glucose-6-phosphate, which can then be further used through glycolysis to produce energy, diverted into the pentose phosphate pathway (PPP) to produce NADPH and anabolic intermediates or converted to glycogen for storage. HK2 is thought to play a key role in promoting anabolic pathways and is frequently overexpressed in cancers (4). Both HK1 and HK2 show cytoplasmic and-through interaction with voltage-dependent anion-selective channel (VDAC)-mitochondrial localization. The presence of HK at the mitochondria provides a close proximity to intramitochondrial ATP production, which helps to couple glycolysis and oxidative phosphorylation (5). This mitochondrial HK also helps to limit mitochondrial reactive oxygen species (ROS) production by maintaining local ADP levels (6). Furthermore, mitochondrial HK2 can directly inhibit apoptosis through regulation of the mitochondrial permeability transition pore that, in part, reflects the ability to block the recruitment of proapoptotic proteins such as Bax and Bak (7-11). The interaction of HK2 with the phosphoprotein PEA15 is also required for protection from apoptosis under hypoxia (12).Severa...

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Section: Resultsmentioning

confidence: 65%

“…However, the ability of TIGAR to promote cell survival is cell and context dependent. In cells that highly depend on the maintenance of glycolytic flux for survival, expression of TIGAR correlates with decreased, rather than increased, survival (16,23).…”

mentioning

confidence: 99%

Mitochondrial localization of TIGAR under hypoxia stimulates HK2 and lowers ROS and cell death

Cheung

Ludwig

Vousden

2012

Proc. Natl. Acad. Sci. U.S.A.

207

168

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“…p53 is responsible for the up-regulation of GLS2, which indirectly generates a-ketoglutarate for the TCA cycle as previously described (36). In addition, the p53-induced factor, TIGAR, is a key inhibitor of glycolysis (48). Structurally, it resembles fructose-2,6-bisphosphatase phosphofructokinase-2 (FBPase-2), the bisphosphatase domain of the bifunctional glycolytic enzyme, PFK-2/FBPase-2; accordingly, TIGAR has been shown to suppress FBPase-2, leading to a marked decrease in glycolytic flux (5).…”

Section: Targeting Glycolysis Via the P53 Signaling Pathwaymentioning

confidence: 73%

Hypoxamirs and Mitochondrial Metabolism

Cottrill

Chan²,

Loscalzo³

2014

Antioxidants & Redox Signaling

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Significance: Chronic hypoxia can drive maladaptive responses in numerous organ systems, leading to a multitude of chronic mammalian diseases. Oxygen homeostasis is intimately linked with mitochondrial metabolism, and dysfunction in these systems can combine to form the backbone of hypoxic-ischemic injury in multiple tissue beds. Increased appreciation of the crucial roles of hypoxia-associated miRNA (hypoxamirs) in metabolism adds a new dimension to our understanding of the regulation of hypoxia-induced disease. Recent Advances: Myriad factors related to glycolysis (e.g., aldolase A and hexokinase II), tricarboxylic acid cycle function (e.g., glutaminase and iron-sulfur cluster assembly protein 1/2), and apoptosis (e.g., p53) have been recently implicated as targets of hypoxamirs. In addition, several hypoxamirs have been implicated in the regulation of the master transcription factor of hypoxia, hypoxia-inducible factor-1a, clarifying how the cellular program of hypoxia is sustained and resolved. Critical Issues: Central to the discussion of metabolic change in hypoxia is the Warburg effect, a shift toward anaerobic metabolism that persists after normal oxygen levels have been restored. Many newly discovered targets of hypoxia-driven microRNA converge on pathways known to be involved in this pathological phenomenon and the apoptosis-resistant phenotype associated with it. Future Directions: The often synergistic functions of miRNA may make them ideal therapeutic targets. The use of antisense inhibitors is currently being considered in diseases in which hypoxia and metabolic dysregulation predominate. In addition, exploration of pleiotripic miRNA functions will likely continue to offer unique insights into the mechanistic relationships of their downstream target pathways and associated hypoxic phenotypes. Antioxid. Redox Signal. 21, 1189-1201.

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“…80 Mitochondrial dysfunction is correlated with two major changes which include changes in the permeabilization of the outer mitochondrial membrane and the loss of the electrochemical gradient. 34,81 Previously, several studies have reported that HDACIs have the potential to trigger depolarization of the mitochondrial membrane, 82,83 which can induce ROS generation. In addition, HDACIs induce the release of proapoptotic Bax and trigger apoptosis via the mitochondrial pathway.…”

Section: Rgo-ag and Tsa Cause Mitochondrial Dysfunctionmentioning

confidence: 99%

Novel biomolecule lycopene-reduced graphene oxide-silver nanoparticle enhances apoptotic potential of trichostatin A in human ovarian cancer cells (SKOV3)

Zhang¹,

Huang²,

Zhang³

et al. 2017

IJN

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Background Recently, there has been much interest in the field of nanomedicine to improve prevention, diagnosis, and treatment. Combination therapy seems to be most effective when two different molecules that work by different mechanisms are combined at low dose, thereby decreasing the possibility of drug resistance and occurrence of unbearable side effects. Based on this consideration, the study was designed to investigate the combination effect of reduced graphene oxide-silver nanoparticles (rGO-AgNPs) and trichostatin A (TSA) in human ovarian cancer cells (SKOV3). Methods The rGO-AgNPs were synthesized using a biomolecule called lycopene, and the resultant product was characterized by various analytical techniques. The combination effect of rGO-Ag and TSA was investigated in SKOV3 cells using various cellular assays such as cell viability, cytotoxicity, and immunofluorescence analysis. Results AgNPs were uniformly distributed on the surface of graphene sheet with an average size between 10 and 50 nm. rGO-Ag and TSA were found to inhibit cell viability in a dose-dependent manner. The combination of rGO-Ag and TSA at low concentration showed a significant effect on cell viability, and increased cytotoxicity by increasing the level of malondialdehyde and decreasing the level of glutathione, and also causing mitochondrial dysfunction. Furthermore, the combination of rGO-Ag and TSA had a more pronounced effect on DNA fragmentation and double-strand breaks, and eventually induced apoptosis. Conclusion This study is the first to report that the combination of rGO-Ag and TSA can cause potential cytotoxicity and also induce significantly greater cell death compared to either rGO-Ag alone or TSA alone in SKOV3 cells by various mechanisms including reactive oxygen species generation, mitochondrial dysfunction, and DNA damage. Therefore, this combination chemotherapy could be possibly used in advanced cancers that are not suitable for radiation therapy or surgical treatment and facilitate overcoming tumor resistance and disease progression.

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p53 and TIGAR regulate cardiac myocyte energy homeostasis under hypoxic stress

Cited by 64 publications

References 39 publications

Mitochondrial localization of TIGAR under hypoxia stimulates HK2 and lowers ROS and cell death

Mitochondrial localization of TIGAR under hypoxia stimulates HK2 and lowers ROS and cell death

Hypoxamirs and Mitochondrial Metabolism

Novel biomolecule lycopene-reduced graphene oxide-silver nanoparticle enhances apoptotic potential of trichostatin A in human ovarian cancer cells (SKOV3)

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