Aging-Dependent Reduction in Glyoxalase 1 Delays Wound Healing

Fleming, Thomas; Theilen, Till M.; Masania, Jinit; Wunderle, Marius; Karimi, Jamshid; Vittas, Spiros; Bernauer, Rainer; Bierhaus, Angelika; Rabbani, Naila; Thornalley, Paul J.; Krøll, Jens; Tyedmers, Jens; Nawrotzki, Ralph; Herzig, Stephan; Brownlee, Michael; Nawroth, Peter P.

doi:10.1159/000351628

Cited by 52 publications

(37 citation statements)

References 52 publications

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“…Our data regarding the effect of Glo1 on kidney and vascular aging are consistent with a recent study showing that age-dependent delay of wound healing is associated with the lowering of Glo1 activity with age [7]. Other studies also indicate that the Glo1 activity of Caenorhabditis elegans decreased by 10% by aging and Glo1 overexpression enhanced their lifespan and, in contrast, Glo1 knockdown significantly shortened the lifespan [8].…”

Section: Glycative Stress In Kidney and Vascular Agingsupporting

confidence: 91%

Glycative stress and glyoxalase in kidney disease and aging

Inagi

2014

Biochemical Society Transactions

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Glycation is one of the important reactions regulating physiological state, and glycative stress, namely an overwhelming and unfavourable glycation state, is established as a pathological factor. Glycative stress is closely associated with not only various kidney diseases, but also kidney aging. Accumulating evidence, including studies in my laboratory, demonstrates that progression of renal tubular damage and its aging is correlated with the decrease in the activity of anti-glycative stress enzyme Glo1 (glyoxalase I) in the kidney. The reduction of glycative and oxidative stresses by Glo1 overexpression is beneficial for prevention of kidney disease and treatment, suggesting the novel therapeutic approaches targeting Glo1. The present review is focused on the impact of glycative stress and Glo1 on protein homoeostasis and discusses further the cross-talk between glycative stress and UPR (unfolded protein response), which controls the protein homoeostasis state.

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Section: Glycative Stress In Kidney and Vascular Agingsupporting

confidence: 91%

Glycative stress and glyoxalase in kidney disease and aging

Inagi

2014

Biochemical Society Transactions

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“…Untreated cells were incubated for the same time periods. Independent experiments were also performed by pretreating cells with N -acetyl- L -cysteine (NAC, 10 m M , for 0.5 h), a known antioxidant that increases cellular GSH levels, aminoguanidine bicarbonate (AG, 1 m M , for 2 h), a scavenger of free MG (Fleming et al , 2013) and MG-derived AGEs (Thornalley et al , 2000), the specific wild-type p53 inhibitor, pifithrin- α (PFT- α , 20 μ M in DMSO, for 2 h), the specific NF-κB inhibitor BAY 11-7082 (10 μ M in DMSO, for 0.5 h, Santa Cruz Biotechnology, Inc., Heidelberg, Germany), the ER α anti-oestrogen ICI 182,780 (100 n M in DMSO, for 4 h), ERK-1/2 inhibitor U-0126 (10 μ M in DMSO, for 1 h), and then irradiated in the conditions above described. Unless otherwise stated, these reagents were from Sigma-Aldrich (Milan, Italy) and used at concentrations producing no significant toxicity to MCF-7 cells.…”

Section: Methodsmentioning

confidence: 99%

Glyoxalase I inhibition induces apoptosis in irradiated MCF-7 cells via a novel mechanism involving Hsp27, p53 and NF-κB

et al. 2014

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Background:Glyoxalase I (GI) is a cellular defence enzyme involved in the detoxification of methylglyoxal (MG), a cytotoxic byproduct of glycolysis, and MG-derived advanced glycation end products (AGEs). Argpyrimidine (AP), one of the major AGEs coming from MG modifications of proteins arginines, is a pro-apoptotic agent. Radiotherapy is an important modality widely used in cancer treatment. Exposure of cells to ionising radiation (IR) results in a number of complex biological responses, including apoptosis. The present study was aimed at investigating whether, and through which mechanism, GI was involved in IR-induced apoptosis.Methods:Apoptosis, by TUNEL assay, transcript and protein levels or enzymatic activity, by RT–PCR, western blot and spectrophotometric methods, respectively, were evaluated in irradiated MCF-7 breast cancer cells, also in experiments with appropriate inhibitors or using small interfering RNA.Results:Ionising radiation induced a dramatic reactive oxygen species (ROS)-mediated inhibition of GI, leading to AP-modified Hsp27 protein accumulation that, in a mechanism involving p53 and NF-κB, triggered an apoptotic mitochondrial pathway. Inhibition of GI occurred at both functional and transcriptional levels, the latter occurring via ERK1/2 MAPK and ERα modulation.Conclusions:Glyoxalase I is involved in the IR-induced MCF-7 cell mitochondrial apoptotic pathway via a novel mechanism involving Hsp27, p53 and NF-κB.

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“…MG-derived AGEs increased in human lens with age and was linked to cataract formation [3]. Decreased Glo1 activity was associated with impaired wound healing [24]. Dicarbonyl stress is also likely involved in senescence of plants.…”

Section: Ageingmentioning

confidence: 99%

Dicarbonyl stress in cell and tissue dysfunction contributing to ageing and disease

Rabbani

Thornalley

2015

Biochemical and Biophysical Research Communications

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Dicarbonyl stress is the abnormal accumulation of dicarbonyl metabolites leading to increased protein and DNA modification contributing to cell and tissue dysfunction in ageing and disease. Enzymes metabolising dicarbonyls, glyoxalase 1 and aldoketo reductases, provide an efficient and stress-response enzyme defence against dicarbonyl stress. Dicarbonyl stress is produced by increased formation and/or decreased metabolism of dicarbonyl metabolites, and by exposure to exogenous dicarbonyls. It contributes to ageing, disease and activity of cytototoxic chemotherapeutic agents.

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Aging-Dependent Reduction in Glyoxalase 1 Delays Wound Healing

Cited by 52 publications

References 52 publications

Glycative stress and glyoxalase in kidney disease and aging

Glycative stress and glyoxalase in kidney disease and aging

Glyoxalase I inhibition induces apoptosis in irradiated MCF-7 cells via a novel mechanism involving Hsp27, p53 and NF-κB

Dicarbonyl stress in cell and tissue dysfunction contributing to ageing and disease

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