Your search keyword '"KÜÇÜKLER, Sefa"' showing total 3 results

1. Protective effects of zingerone against sodium arsenite-induced lung toxicity: A multi-biomarker approach.

Author

Şimşek, Hasan, Küçükler, Sefa, Gür, Cihan, İleritürk, Mustafa, Aygörmez, Serpil, and Kandemir, Fatih Mehmet

Subjects

*LUNGS, *SODIUM arsenite, *OXIDATIVE stress, *SODIUM, *HONEY plants

Abstract

Objective(s): Sodium arsenite (SA) exposure is toxic to the body. Zingerone (ZNG) is a flavonoid with many biological properties found naturally in honey and plants. This study aimed to determine the effects of ZNG on SA-induced rat lung toxicity. Materials and Methods: Thirty-five male Sprague rats were divided into Control, SA, ZNG, SA+ZNG25, and SA+ZNG50 groups (n=7). SA 10 mg/kg and ZNG were administered at two doses (25 and 50 mg/kg) (orally, 14 days). Analysis of oxidative stress, inflammation damage, apoptosis damage, and autophagic damage markers in lung tissue were determined by biochemical and histological methods. Results: The administration of ZNG reduced oxidative stress by increasing SA-induced decreased antioxidant enzyme activities, increasing Nrf-2, HO-1, and NQO1, and decreasing MDA level. ZNG administration reduced inflammation marker levels. Anti-apoptotic Bcl-2 increased and apoptotic Bax and Caspase-3 decreased with ZNG. ZNG promoted the regression of autophagy by reducing Beclin-1, LC3A, and LC3B levels. Conclusion: Evaluating all data showed that SA caused toxic damage to lung tissue by increasing inflammation, apoptosis, autophagy, and oxidant levels, whereas ZNG had a protective effect by reducing this damage. [ABSTRACT FROM AUTHOR]

Published

2023

2. The investigation of the effect of fraxin on hepatotoxicity induced by cisplatin in rats.

Author

Ekinci-Akdemir, Fazile Nur, Bingöl, Çiğdem, Yıldırım, Serkan, Kandemir, Fatih Mehmet, Küçükler, Sefa, and Sağlam, Yavuz Selim

Subjects

HEPATOTOXICOLOGY, CISPLATIN, RATS, LIVER injuries

Abstract

Objective(s): This study was designed to assess the effect of fraxin which has various biological properties against liver injury induced by cisplatin. Materials and Methods: In our study, 24 Wistar albino rats were randomly assigned to control, fraxin, cisplatin, and fraxin+cisplatin groups. Cisplatin 12 mg/kg IP and fraxin 40 mg/kg orally were applied. When the experiment ended, the rats were sacrificed and the liver tissues were taken rapidly. Liver tissue specimens were maintained under appropriate conditions. Later, biochemical, histopathological, and immunohistochemical evaluations were performed. Results: According to our biochemical findings, oxidant parameters increased while antioxidant parameters decreased in cisplatin group compared with control group. Antioxidant parameters increased but oxidant parameters decreased in fraxin + cisplatin group compared with the cisplatin group. Immunohistochemical evaluations showed that the expressions of TNF-a and Caspase-3 were negative in control and fraxin groups, whereas severe levels were found in the cisplatin group. However, it was determined that the expressions of TNF-a and Caspase-3 were in mild levels in fraxin + cisplatin treatment group. In addition, it was observed that the increase of pathological markers such as coagulation necrosis, hydropic degeneration, dilatation in sinusoid, and hyperemia in the cisplatin group were compatible with our biochemical and immunohistochemical findings. Conclusion: Biochemical, immunohistochemical, and histopathological results revealed that fraxin was effective in relieving cisplatin-induced liver damage. [ABSTRACT FROM AUTHOR]

Published

2020

3. The effects of casticin and myricetin on liver damage induced by methotrexate in rats.

Author

Ekinci-Akdemir, Fazile Nur, Yildirim, Serkan, Kandemir, Fatih Mehmet, Gülçin, İlhami, Küçükler, Sefa, Sağlam, Yavuz Selim, and Yakan, Selvinaz

Subjects

MYRICETIN, METHOTREXATE, LABORATORY rats, MALONDIALDEHYDE, LIVER cells

Abstract

Objective(s): : In this study, we evaluated the therapeutic effects of casticin and myricetin on liver damage induced by methotrexate in rats. Materials and Methods: Thirty-six male rats were used for the study and divided into 6 groups: control, methotrexate, casticin, myricetin, casticin+methotrexate, and myricetin+methotrexate. It was performed by methotrexate (20 mg/kg single dose, IP) in methotrexate, casticin+methotrexate and myricetin+methotrexate groups. Casticin 200 mg/kg dose was given to casticin and casticin+methotrexate groups. Myricetin 50 mg/kg dose was given to myricetin and myriceytin+methotrexate groups. At the end of the experiment, liver tissues were removed for the purpose of histopathological, biochemical and immunohistochemical assessments. Results: In our study, we have detected that MDA levels increased and activities of antioxidant enzymes SOD, CAT, and GPX decreased in the methotrexate group compared to the other groups, but the level of MDA decreased and activities of these enzymes increased in casticin+methotrexate and myricetin+methotrexate groups compared to the methotrexate group. In immunohistochemical examinations of control, casticin and myricetin groups in liver tissues no caspase-3 and 8-OHdG expressions were observed. In the MTX group, caspase-3 and 8-OHdG expressions were seen at the severe levels. Caspase-3 and 8-OHdG expressions were mild in hepatocytes in the casticin+methotrexate and myricetin+methotrexate groups. When the liver tissues of the rats in the methotrexate group were examined, severe pathological damage was detected both in the parietal region and in the portal region. Conclusion: By looking at these results, we can say that casticin and myricetin are effective against liver damage induced by methotrexate. [ABSTRACT FROM AUTHOR]

Published

2018