4.7 Article

The Protective Effect of Exogenous 17β-Estradiol against Experimentally Induced Oxidative Damage to Membrane Lipids Is Stronger in Male vs. Female Porcine Thyroids: Preliminary Results

Journal

TOXICS
Volume 11, Issue 9, Pages -

Publisher

MDPI
DOI: 10.3390/toxics11090746

Keywords

17 beta-estradiol; thyroid; oxidative stress; Fenton reaction; sexual dimorphism

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This study aimed to examine the effects of 17 beta-estradiol on oxidative damage to membrane lipids in relation to sex differences in thyroid function. Results showed that 17 beta-estradiol did not affect lipid peroxidation in thyroid homogenates under basal conditions, but it had a stronger protective effect in male thyroids compared to female thyroids.
It is well-known that thyroid diseases are more prevalent in women than in men. The contribution of sex hormones may explain such disparity. The aim of this study was to check if there are any differences between sexes concerning the effects of 17 beta-estradiol on oxidative damage to membrane lipids (lipid peroxidation) in porcine thyroid homogenates under basal conditions and in the presence of Fenton reaction (Fe2+ + H2O2 -> Fe3+ + (OH)-O-center dot + OH-) substrates. We observed that 17 beta-estradiol did not change the basal level of lipid peroxidation (measured spectrophotometrically as concentrations of malondialdehyde + 4-hydroxyalkenals) in thyroid homogenates, and no differences were found between sexes. The lipid peroxidation level in response to Fe2+ + H2O2 plus 17 beta-estradiol was lower in male thyroids. In turn, in male thyroids, 17 beta-estradiol reduced experimentally induced lipid peroxidation in as low of a concentration as 0.1 mu M, whereas in female thyroids the lowest effective concentration of 17 beta-estradiol was 10 mu M, i.e., 100 times higher than in males. In conclusion, the protective effects of exogenous 17 beta-estradiol against experimentally induced oxidative damage to membrane lipids is stronger in male than in female thyroids. Our observation suggests that female tissue is less sensitive to the protective effects of exogenous 17 beta-estradiol. This sexual dimorphism of oxidative processes in the thyroid may constitute one of the mechanisms of the different prevalence of thyroid diseases in women and in men.

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