Your search keyword '"Petrik, József"' showing total 6 results

1. Flavonoid diosmetin increases ATP levels in kidney cells and relieves ATP depleting effect of ochratoxin A.

Author

Poór M, Veres B, Jakus PB, Antus C, Montskó G, Zrínyi Z, Vladimir-Knežević S, Petrik J, and Kőszegi T

Subjects

ATP Synthetase Complexes antagonists & inhibitors, ATP Synthetase Complexes metabolism, Animals, Cell Survival drug effects, Dogs, Flavonoids chemistry, Hep G2 Cells, Humans, Kidney cytology, Kidney metabolism, Madin Darby Canine Kidney Cells, Mitochondria, Liver drug effects, Mitochondria, Liver metabolism, Rats, Reactive Oxygen Species metabolism, Adenosine Triphosphate metabolism, Flavonoids pharmacology, Kidney embryology, Ochratoxins toxicity

Abstract

Diosmetin (DIOS) is a flavone aglycone commonly occurring in citrus species and olive leaves, in addition it is one of the active ingredients of some medications. Based on both in vitro and in vivo studies several beneficial effects are attributed to DIOS but the biochemical background of its action seems to be complex and it has not been completely explored yet. Previous investigations suggest that most of the flavonoid aglycones have negative effect on ATP synthesis in a dose dependent manner. In our study 17 flavonoids were tested and interestingly DIOS caused a significant elevation of intracellular ATP levels after 6- and 12-h incubation in MDCK kidney cells. In order to understand the mechanism of action, intracellular ATP and protein levels, ATP/ADP ratio, cell viability and ROS levels were determined after DIOS treatment. In addition, impacts of different enzyme inhibitors and effect of DIOS on isolated rat liver mitochondria were also tested. Finally, the influence of DIOS on the ATP depleting effect of the mycotoxin, ochratoxin A was also investigated. Our major conclusions are the followings: DIOS increases intracellular ATP levels both in kidney and in liver cells. Inhibition of glycolysis or citric acid cycle does not decrease the observed effect. DIOS-induced elevation of ATP levels is completely abolished by the inhibition of ATP synthase. DIOS is able to completely reverse the ATP-depleting effect of the mycotoxin, ochratoxin A. Most probably the DIOS-induced impact on ATP system does not originate from the antioxidant property of DIOS. Based on our findings DIOS may be promising agent to positively influence ATP depletion caused by some metabolic poisons., (Copyright © 2014 Elsevier B.V. All rights reserved.)

Published

2014

2. Fluorescence spectroscopic investigation of competitive interactions between ochratoxin A and 13 drug molecules for binding to human serum albumin.

Author

Poór M, Kunsági-Máté S, Czibulya Z, Li Y, Peles-Lemli B, Petrik J, Vladimir-Knežević S, and Kőszegi T

Subjects

Binding Sites, Humans, Spectrometry, Fluorescence, Ochratoxins chemistry, Pharmaceutical Preparations chemistry, Serum Albumin chemistry

Abstract

Ochratoxin A (OTA) is a highly toxic mycotoxin found worldwide in cereals, foods, animal feeds and different drinks. Based on previous studies, OTA is one of the major causes of the chronic tubulointerstitial nephropathy known as Balkan endemic nephropathy (BEN) and exerts several other adverse effects shown by cell and/or animal models. It is a well-known fact that OTA binds to various albumins with very high affinity. Recently, a few studies suggested that reducing the bound fraction of OTA might reduce its toxicity. Hypothetically, certain drugs can be effective competitors displacing OTA from its albumin complex. Therefore, we examined 13 different drug molecules to determine their competing abilities to displace OTA from human serum albumin (HSA). Competitors and ineffective chemicals were identified with a steady-state fluorescence polarization-based method. After characterization the competitive abilities of individual drugs, drug pairs were formed and their displacing activity were tested in OTA-HSA system. Indometacin, phenylbutazone, warfarin and furosemide showed the highest competing capacity but ibuprofen, glipizide and simvastatin represented detectable interaction too. Investigations of drug pairs raised the possibility of the presence of diverse binding sites of competing drugs. Apart from the chemical information obtained in our model, this explorative research might initiate future designs for epidemiologic studies to gain further in vivo evidence of long-term (potentially protective) effects of competing drugs administered to human patients., (Copyright © 2012 John Wiley & Sons, Ltd.)

Published

2013

3. Flavonoid aglycones can compete with Ochratoxin A for human serum albumin: a new possible mode of action.

Author

Poór M, Kunsági-Máté S, Bencsik T, Petrik J, Vladimir-Knežević S, and Kőszegi T

Subjects

Binding, Competitive, Flavonoids metabolism, Humans, Ochratoxins metabolism, Protein Binding, Flavonoids chemistry, Ochratoxins chemistry, Serum Albumin metabolism

Abstract

The mycotoxin Ochratoxin A (OTA) appears worldwide in cereals, plant products, different foods and drinks. Ochratoxin A binds to plasma albumin with a very high affinity. However, it is well known that natural flavonoids can also bind to human serum albumin (HSA) at the same binding site as OTA does (site I, subdomain IIA). A few experimental literature data suggest that reducing the bound fraction of OTA speeds up its elimination rate with a potential decrease in its toxicity. In our experimental model competitive binding properties of flavonoid aglycones were examined with a fluorescence polarization based approach. Our data show that some of the flavonoids are able to remove the toxin from HSA. We conclude that among the 13 studied flavonoid aglycones galangin and quercetin were the most effective competitors for OTA., (Copyright © 2012 Elsevier B.V. All rights reserved.)

Published

2012

4. Lipid peroxidation and glutathione levels in porcine kidney PK15 cells after individual and combined treatment with fumonisin B(1), beauvericin and ochratoxin A.

Author

Klarić MS, Pepeljnjak S, Domijan AM, and Petrik J

Subjects

Animals, Carcinogens administration & dosage, Cell Survival drug effects, Cells, Cultured, Depsipeptides administration & dosage, Drug Interactions, Enzyme Inhibitors administration & dosage, Epithelial Cells drug effects, Fumonisins administration & dosage, Glutathione drug effects, Kidney cytology, Kidney drug effects, Lipid Peroxidation drug effects, Ochratoxins administration & dosage, Swine, Carcinogens pharmacology, Depsipeptides pharmacology, Enzyme Inhibitors pharmacology, Fumonisins pharmacology, Ochratoxins pharmacology

Abstract

Individual and combined effects of the mycotoxins fumonisin B(1), beauvericin and ochratoxin A on cell viability, lipid peroxidation (TBARS) and intracellular glutathione (GSH) were studied on porcine kidney epithelial cells (PK15). Cells were treated with 0.05, 0.5 and 5 microg/ml of each mycotoxin or the combinations of two or all three applied in equal concentrations for 24 and 48 hr. Changes in cell viability, GSH and TBARS levels showed that the cytotoxic effects of these mycotoxins were concentration- and time-dependent. After 24 hr, cell viability was significantly decreased by the exposure to 5 microg/ml of fumonisin B(1) (25%), beauvericin (30%) and ochratoxin A (35%), as compared to controls. Only ochratoxin A (5 microg/ml) increased TBARS (56%), with further significant increase (85%) after 48 hr exposure. Fumonisin B(1) and beauvericin significantly increased TBARS (57% and 80%, respectively) only when the highest dose was applied for 48 hr. After 24 hr, GSH was significantly decreased (18%) by ochratoxin A (0.05 microg/ml), whereas fumonisin B(1) and beauvericin significantly decreased GSH at the concentration of 0.5 microg/ml. Combined treatment with fumonisin B(1), beauvericin and ochratoxin A resulted mostly in additive effects especially after a 24-hr exposure, although synergistic as well as antagonistic interactions could not be excluded depending on toxin concentrations and time of exposure. This is the first report on beauvericin-induced effects on lipid peroxidation and GSH in animal cells.

Published

2007

5. Apoptosis and oxidative stress induced by ochratoxin A in rat kidney.

Author

Petrik J, Zanić-Grubisić T, Barisić K, Pepeljnjak S, Radić B, Ferencić Z, and Cepelak I

Subjects

Animals, Antioxidants metabolism, In Vitro Techniques, Kidney enzymology, Kidney metabolism, Lipid Peroxidation drug effects, Male, Malondialdehyde metabolism, Rats, Rats, Wistar, Superoxide Dismutase metabolism, Apoptosis, Kidney drug effects, Mycotoxins toxicity, Ochratoxins toxicity, Oxidative Stress

Abstract

Ochratoxin A (OTA) is a widespread mycotoxin produced by several species of fungi. OTA induces a tubular-interstitial nephropathy in humans and in animals. It has been implicated as one of the aetiological agents involved in the development of endemic nephropathy. OTA-induced oxidative stress and apoptosis may play key roles in the development of chronic tubulointerstitial nephritis connected to the long-term exposure to this food contaminant. We studied the effects of low doses of OTA on kidney cells. Wistar rats were treated with 120 microg OTA/kg bodyweight daily, for 10, 30 or 60 days. Toxin concentration in kidney was proportional to the time of exposure, and amounted to 547.2, 752.5 and 930.3 ng OTA/g kidney tissue after 10, 30 and 60 days, respectively. OTA treatment caused an increased number of cells undergoing apoptosis in both proximal and distal epithelial kidney cells. The apoptotic cells were visualised using the TUNEL assay and staining with haematoxylin and eosin in situ. The number of apoptotic cells in rats treated for 10, 30 and 60 days increased by 5-, 6.4- and 12.7-fold, respectively, compared with the control cells. However, DNA electrophoresis did not show characteristic fragmentation (DNA laddering). The oxidative stress was evident via increased malondialdehyde formation. The concentration of lipid peroxides showed an increase (36%), but the activity of superoxide dismutase decreased (26%) in 60-day treated rats. In spite of the observed biochemical and morphological changes in the kidney cells, renal functional status was preserved to the end of experiment. This study demonstrates that a combination of morphologic and biochemical markers can be used to monitor early cell death in OTA-induced renal injury. We have shown that the exposure to the relatively low OTA concentrations has activated apoptotic processes and oxidative damage in kidney cells.

Published

2003

6. Lipid Peroxidation and Glutathione Levels in Porcine Kidney PK15 Cells after Individual and Combined Treatment with Fumonisin B1, Beauvericin and Ochratoxin A.

Author

Klarić, Maja Šegvić, Pepeljnjak, Stjepan, Domijan, Ana-Marija, and Petrik, József

Subjects

RENAL pharmacology, MYCOTOXINS, FUMONISINS, OCHRATOXINS, PEROXIDATION, GLUTATHIONE

Abstract

Individual and combined effects of the mycotoxins fumonisin B1, beauvericin and ochratoxin A on cell viability, lipid peroxidation (TBARS) and intracellular glutathione (GSH) were studied on porcine kidney epithelial cells (PK15). Cells were treated with 0.05, 0.5 and 5 µg/ml of each mycotoxin or the combinations of two or all three applied in equal concentrations for 24 and 48 hr. Changes in cell viability, GSH and TBARS levels showed that the cytotoxic effects of these mycotoxins were concentration- and time-dependent. After 24 hr, cell viability was significantly decreased by the exposure to 5 µg/ml of fumonisin B1 (25%), beauvericin (30%) and ochratoxin A (35%), as compared to controls. Only ochratoxin A (5 µg/ml) increased TBARS (56%), with further significant increase (85%) after 48 hr exposure. Fumonisin B1 and beauvericin significantly increased TBARS (57% and 80%, respectively) only when the highest dose was applied for 48 hr. After 24 hr, GSH was significantly decreased (18%) by ochratoxin A (0.05 µg/ml), whereas fumonisin B1 and beauvericin significantly decreased GSH at the concentration of 0.5 µg/ml. Combined treatment with fumonisin B1, beauvericin and ochratoxin A resulted mostly in additive effects especially after a 24-hr exposure, although synergistic as well as antagonistic interactions could not be excluded depending on toxin concentrations and time of exposure. This is the first report on beauvericin-induced effects on lipid peroxidation and GSH in animal cells. [ABSTRACT FROM AUTHOR]

Published

2007