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Effects of naringin and valproate interaction on liver steatosis and dyslipidaemia parameters in male C57BL6 mice (CROSBI ID 308043)

Prilog u časopisu | izvorni znanstveni rad | međunarodna recenzija

Jutrić, David ; Đikić, Domagoj ; Boroš, Almoš ; Odeh, Dyana ; Domjanić Drozdek, Sandra ; Gračan, Romana ; Dragičević, Petar ; Crnić, Irena ; Landeka Jurčević, Irena Effects of naringin and valproate interaction on liver steatosis and dyslipidaemia parameters in male C57BL6 mice // Arhiv za higijenu rada i toksikologiju, 73 (2022), 71-82. doi: 10.2478/aiht-2022-73-3608

Podaci o odgovornosti

Jutrić, David ; Đikić, Domagoj ; Boroš, Almoš ; Odeh, Dyana ; Domjanić Drozdek, Sandra ; Gračan, Romana ; Dragičević, Petar ; Crnić, Irena ; Landeka Jurčević, Irena

engleski

Effects of naringin and valproate interaction on liver steatosis and dyslipidaemia parameters in male C57BL6 mice

Valproate is a common antiepileptic drug whose adverse effects include liver steatosis and dyslipidaemia. The aim of our study was to see how natural flavonoid antioxidant naringin would interact with valproate and attenuate these adverse effects. For this reason we treated male C57BL6 mice with a combination of 150 mg/kg of valproate and 25 mg/kg naringin every day for 10 days and compared their serum triglycerides, cholesterol, LDL, HDL, VLDL, and liver PPAR-alpha, PGC-1 alpha, ACOX1, Nrf2, SOD, CAT, GSH, and histological signs of steatosis. Valproate increased lipid peroxidation parameters and caused pronounced microvesicular steatosis throughout the hepatic lobule in all acinar zones, but naringin co-administration limited steatosis to the lobule periphery. In addition, it nearly restored total serum cholesterol, LDL, and triglycerides and liver ACOX1 and MDA to control levels. and upregulated PPAR-alpha and PGC-1 alpha, otherwise severely downregulated by valproate. It also increased SOD activity. All these findings suggest that naringin modulates key lipid metabolism regulators and should further be investigated in this model, either alone or combined with other lipid regulating drugs or molecules.

ACOX1, cholesterol, dyslipidaemia, lipid regulating transcription factors, Nrf2, oxidative stress, PPAR-alpha, PGC-1 alpha

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Podaci o izdanju

73

2022.

71-82

objavljeno

0004-1254

1848-6312

10.2478/aiht-2022-73-3608

Povezanost rada

Biologija

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