MORPHOLOGICAL CHANGES AND OXIDATIVE HOMEOSTASIS IN THE LIVER TISSUES DURING LONG CENTRAL DEPRIVATION OF LUTEINIZING HORMONE SYNTHESIS BY TRIPTORELIN

O. A. Polyvyana, V. Shepitko, Y. Stetsuk, O. Akimov, O. S. Yakushko, O. Voloshyna
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引用次数: 1

Abstract

In recent years, researchers have focused on the problem of the dependence of the functioning of various organs and systems on the level of androgens. The effect of long inhibition of testosterone synthesis by triptorelin on liver tissue is poorly understood. The aim of this research was to establish the microscopic organization of rat livers, production of nitric oxide and the intensity of oxidative stress in the rat livers during experimental central deprivation of luteinizing hormone synthesis by diphereline injection on the 270-360th day of the experiment. The experiments were carried out on 30 sexually mature male white rats of the Wistar line. Rats were divided into 2 groups: the control group (10) and the experimental group (20). Animals from the experimental group were subcutaneously injected triptorelin at a dose of 0.3 mg of the active substance/ per kg of body weight for 360 days, while the control group received an injection of saline. It was found that oxidative stress develops in hepatocytes, which is morphologically confirmed by karyopyknosis of the nuclei, oxyphilia of the cytoplasm with the appearance of a significant number of vacuoles in it. The vessels of the microcirculatory bed react with stasis. An increase in the production of superoxide radical anion in rat liver may be due to the absence of an inhibitory effect of testosterone on macrophages and liver mitochondria, which is accompanied by depletion of antioxidant enzymes and the development of oxidative stress. The intensity of biochemical markers of oxidative stress on the 360th day is lower than on the 270th day, which is due to an increase in the activity of antioxidant enzymes and a decrease in the production of reactive oxygen species.
曲普瑞林长期中枢剥夺黄体生成素合成过程中肝组织的形态学变化及氧化稳态
近年来,研究人员一直关注各种器官和系统的功能对雄激素水平的依赖性问题。曲普瑞林长期抑制睾酮合成对肝组织的影响尚不清楚。本研究的目的是建立大鼠肝脏的微观组织、一氧化氮的产生以及大鼠肝脏在实验的270-360天通过双哌啉注射进行的黄体生成激素合成的实验性中枢剥夺过程中的氧化应激强度。实验在Wistar系的30只性成熟雄性大鼠上进行。将大鼠分为2组:对照组(10只)和实验组(20只)。来自实验组的动物以0.3mg活性物质/kg体重的剂量皮下注射曲普瑞林360天,而对照组接受盐水注射。研究发现,肝细胞中会产生氧化应激,这在形态学上可通过细胞核的核固缩、细胞质的嗜氧性和大量液泡的出现得到证实。微循环床的血管会发生停滞反应。大鼠肝脏中超氧化物自由基阴离子产生的增加可能是由于睾酮对巨噬细胞和肝线粒体没有抑制作用,这伴随着抗氧化酶的耗竭和氧化应激的发展。氧化应激的生化标志物在第360天的强度低于第270天,这是由于抗氧化酶的活性增加和活性氧的产生减少。
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