Dihydroquercetin and biochaga reduce H2O2-induced DNA damage in peripheral blood mononuclear cells of obese women in vitro—a pilot study

Author:

Živković Lada1,Pirković Andrea2ORCID,Topalović Dijana1,Borozan Sunčica3,Bajić Vladan4,Srećković Vesna Dimitrijević5,Djelić Ninoslav6,Petrović Hristina7,Milić Mirta8ORCID,Spremo-Potparević Biljana1

Affiliation:

1. Department of Pathobiology, Faculty of Pharmacy, University of Belgrade , 11000, Belgrade , Serbia

2. Department for Biology of Reproduction, University of Belgrade, Institute for Application of Nuclear Energy , 11000, Belgrade , Serbia

3. Department of Chemistry, University of Belgrade, Faculty of Veterinary Medicine , 11000, Belgrade , Serbia

4. Laboratory for Radiobiology and Molecular Genetics, University of Belgrade, Institute for Nuclear Research ‘Vinča’ , 11000, Belgrade , Serbia

5. Faculty of Medicine, Clinic for Endocrinology, Diabetes and Metabolic Diseases, University of Belgrade , 11000, Belgrade , Serbia

6. Department of Biology, University of Belgrade, Faculty of Veterinary Medicine , 11000, Belgrade , Serbia

7. Faculty of Medicine, University of Belgrade, University Children’s Hospital , 11000, Belgrade , Serbia

8. Mutagenesis Unit, Institute for Medical Research and Occupational Health , 10000, Zagreb , Croatia

Abstract

Abstract Systemic oxidative stress stemming from increased free radical production and reduced antioxidant capacity are common characteristics of obese individuals. Using hydrogen peroxide (H2O2) to induce DNA damage in vitro, in peripheral blood mononuclear cells (PBMCs) from obese subjects and controls, the DNA protective ability of dihidroqercetin (DHQ) and biochaga (B) alone or in combination, were evaluated. The effects of DHQ and B were estimated under two experimental conditions: pre-treatment, where cells were pre-incubated with the substances prior to H2O2 exposure; and post-treatment when cells were first exposed to H2 H2O2, and further treated with the compounds. DNA damage was evaluated using the comet assay. The results of pre- and post-treatment showed a significant decrease in DNA damage produced by H2O2 in the obese group. This decrease was not significant in control group probably due to a small number of subjects in this pilot study. More prominent attenuation was noted in the pre-treatment with DHQ (250 μg/ml). Analysis of antioxidant properties revealed that DHQ’s remarkable reducing power, 1,1-diphenyl-2-picrylhydrazyl (DPPH) scavenging activity, and potent∙OH scavenging properties may contribute to strong attenuation of H2O2-induced DNA damage. Also, B showed strong reducing power, DPPH, and ∙OH scavenging ability, while reducing power and DPPH scavenger effects were increased in the presence of DHQ. Conclusively, DHQ and B may reduce H2O2-induced DNA damage in PBMCs from obese subjects when challenged in vitro, and could be valuable tools in future research against oxidative damage-related conditions.

Publisher

Oxford University Press (OUP)

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