Abstract

Hashimoto’s thyroiditis (HT) is one of the most common autoimmune diseases. Although HT is inextricably linked to oxidative stress, there have been no studies assessing salivary redox homeostasis or salivary gland function in patients with HT. This study is the first to compare antioxidant defense and oxidative stress biomarkers in non-stimulated (NWS) and stimulated (SWS) whole saliva and plasma/erythrocytes of HT patients compared to controls. The study included 45 women with HT in the euthyreosis period as well as an age- and gender-matched control group. We showed that NWS secretion was significantly lower in HT patients compared to healthy controls, similar to salivary amylase activity in NWS and SWS. Catalase and peroxidase activities were considerably higher in NWS and SWS of HT patients, while the concentrations of reduced glutathione and uric acid were significantly lower in comparison with healthy subjects. Total antioxidant potential was significantly lower, while total oxidant status and the level of oxidation products of proteins (advanced glycation end products, advanced oxidation protein products) and lipids (malondialdehyde, lipid hydroperoxides) were significantly higher in NWS, SWS and plasma of HT patients. In conclusion, in both salivary glands of women with HT in euthyreosis, the ability to maintain redox homeostasis was hindered. In HT patients we observed oxidative damage to salivary proteins and lipids; thus, some biomarkers of oxidative stress may present a potential diagnostic value.

Highlights

  • Hashimoto’s disease (HT) is known as chronic lymphocytic thyroiditis

  • Salivary amylase activity was considerably lower in NWS (↓50%, p = 0.00001) and stimulated (NWS) and stimulated (SWS) (↓114%, p = 0.00001) of HT patients compared to the controls (Table 2)

  • In the presented experiment we employed a wide range of biochemical assays to search for a link between oxidative stress (OS) expressed as antioxidant activity/concentration and oxidative damage products and salivary gland function in patients with HT in euthyreosis

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Summary

Introduction

Hashimoto’s disease (HT) is known as chronic lymphocytic thyroiditis. It is an autoimmune-mediated disease characterized by dense infiltrations of the thyroid gland by plasma cells, macrophages and, lymphocytes [1,2]. OS is a situation in which balance between reactive oxygen species (ROS) and the body’s ability to neutralize them is shifted in favor of oxidants [5]. This leads to a temporary or chronic elevation of ROS concentration as well as disturbed cell metabolism and degradation of cell components [5]

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