Signal Transduction by Mitochondrial Oxidants

Finkel, Toren

doi:10.1074/jbc.r111.271999

Cited by 347 publications

(247 citation statements)

References 57 publications

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“…To understand the mechanism of this induction, we explored a role for ROS, which have been shown to stabilize HIF1a. 10,18 Treatment of cells with NAC confirmed a critical role for ROS, as this antioxidant completely blocked 0.1 Gy-induced increase of HIF1a (Figure 4d). A requirement of HIF1a in 0.1 Gy-induced expression of glycolytic genes (Figure 4e), and GLUT-1 and 3 (Figure 4f) was demonstrated by HIF1a knockdown.…”

Section: Resultsmentioning

confidence: 69%

“…9 When mildly increased, ROS, however, can function as signal molecules modulating cellular physiology. 10,11 ROS act through oxidation of reactive cysteine residues in specific target proteins controlling various signaling cascades. A prototype of the ROS-susceptible proteins is phosphatases.…”

mentioning

confidence: 99%

“…For instance, the NFkB pathway stimulates transcription of HIF-1a, 16,17 the PI3K/AKT/mTOR pathway promotes HIF-1a mRNA translation 18 and ROS inhibits HIF-1a degradation. 10 Upon induction, HIF-1a stimulates transcription of genes encoding glucose transporters and enzymes of glycolysis and the pentose phosphate pathway (PPP). 19,20 HIF-1a also negatively regulates TCA cycle enzymes, indirectly through inducing miR120.…”

mentioning

confidence: 99%

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Low-dose radiation exposure induces a HIF-1-mediated adaptive and protective metabolic response

et al. 2014

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Because of insufficient understanding of the molecular effects of low levels of radiation exposure, there is a great uncertainty regarding its health risks. We report here that treatment of normal human cells with low-dose radiation induces a metabolic shift from oxidative phosphorylation to aerobic glycolysis resulting in increased radiation resistance. This metabolic change is highlighted by upregulation of genes encoding glucose transporters and enzymes of glycolysis and the oxidative pentose phosphate pathway, concomitant with downregulation of mitochondrial genes, with corresponding changes in metabolic flux through these pathways. Mechanistically, the metabolic reprogramming depends on HIF1a, which is induced specifically by lowdose irradiation linking the metabolic pathway with cellular radiation dose response. Increased glucose flux and radiation resistance from low-dose irradiation are also observed systemically in mice. This highly sensitive metabolic response to lowdose radiation has important implications in understanding and assessing the health risks of radiation exposure.

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Section: Resultsmentioning

confidence: 69%

mentioning

confidence: 99%

mentioning

confidence: 99%

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Low-dose radiation exposure induces a HIF-1-mediated adaptive and protective metabolic response

et al. 2014

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“…[2][3][4][5] Mitochondria play a key role in maintaining the homeostasis of cells in response to IR, and function as a central platform for cellular signaling. 6 Mitochondria-mediated cellular signaling, including Mn-superoxide dismutase (MnSOD) and nuclear factor kB (NF-kB), is associated with the nontargeted effects of IR, such as the adaptive response, bystander effect, and genomic instability. 7,8 Upon high dose of IR, mitochondria release cytochrome c to induce apoptosis in irradiated cells.…”

Section: Introductionmentioning

confidence: 99%

A comparison of radiation-induced mitochondrial damage between neural progenitor stem cells and differentiated cells

et al. 2017

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Mitochondria play a key role in maintaining cellular homeostasis during stress responses, and mitochondrial dysfunction contributes to carcinogenesis, aging, and neurologic disease. We here investigated ionizing radiation (IR)-induced mitochondrial damage in human neural progenitor stem cells (NSCs), their differentiated counterparts and human normal fibroblasts. Long-term fractionated radiation (FR) with low doses of X-rays for 31 d enhanced mitochondrial activity as evident by elevated mitochondrial membrane potential (DCm) and mitochondrial complex IV (cytochrome c oxidase) activity to fill the energy demands for the chronic DNA damage response in differentiated cells. Subsequent reduction of the antioxidant glutathione via continuous activation of mitochondrial oxidative phosphorylation caused oxidative stress and genomic instability in differentiated cells exposed to longterm FR. In contrast, long-term FR had no effect on the mitochondrial activity in NSCs. This cell type showed efficient DNA repair, no mitochondrial damage, and resistance to long-term FR. After high doses of acute single radiation (SR) (> 5 Gy), cell cycle arrest at the G2 phase was observed in NSCs and human fibroblasts. Under this condition, increase in mitochondria mass, mitochondrial DNA, and intracellular reactive oxygen species (ROS) levels were observed in the absence of enhanced mitochondrial activity. Consequently, cellular senescence was induced by high doses of SR in differentiated cells.In conclusion, we demonstrated that mitochondrial radiation responses differ according to the extent of DNA damage, duration of radiation exposure, and cell differentiation.

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“…However, under certain normoxia conditions, HIF-1␣ expression can also be increased. For instance, the NFB pathway stimulates transcription of HIF-1␣ (6,7), the PI3K/AKT/mammalian target of rapamycin pathway promotes HIF-1␣ mRNA translation (5), and reactive oxygen species inhibit HIF-1␣ degradation (8,9). Upon induction, HIF-1␣ stimulates the transcription of genes encoding glucose transporters and enzymes of glycolysis and the pentose phosphate pathway (2,3).…”

mentioning

confidence: 99%

A Low-dose Arsenic-induced p53 Protein-mediated Metabolic Mechanism of Radiotherapy Protection

Ganapathy

Xiao

Yang

et al. 2014

Journal of Biological Chemistry

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Background: Radiotherapy protection depends on a selective protection of normal tissues but not tumors. Results: We demonstrate that low doses of arsenic induce a p53/HIF-1␣-dependent metabolic reprogramming specific to normal cells, resulting in increased resistance to radiation toxicity. Conclusion: p53-mediated metabolic reprogramming can be explored for normal tissue protection. Significance: The use of low-dose arsenic for selective protection of normal tissues may have important therapeutic implications.

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Signal Transduction by Mitochondrial Oxidants

Cited by 347 publications

References 57 publications

Low-dose radiation exposure induces a HIF-1-mediated adaptive and protective metabolic response

Low-dose radiation exposure induces a HIF-1-mediated adaptive and protective metabolic response

A comparison of radiation-induced mitochondrial damage between neural progenitor stem cells and differentiated cells

A Low-dose Arsenic-induced p53 Protein-mediated Metabolic Mechanism of Radiotherapy Protection

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