PARKINSONISM SYNDROME FORMATION IN EXPERIMENTAL ANIMALS. NEUROINFLAMMATORY PENUMBRA

A. Boika, N. Aleinikava, V. Ponomarev, A. M. Ustsiamchuk, H. Ivanchik
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Abstract

Much valuable information about the development of Parkinson’s disease (PD) has been obtained from studies on the laboratory animals. Objectives. To compare the development of neurotoxic and neuroinflammatory parkinsonism syndrome in laboratory animals. Material and methods. The number of rats in the group of neuroinflammatory model of parkinsonism syndrome (lipopolysaccharide) was 6, and in the group of neurotoxic model (rotenone) - 20. The control group consisted of 5 animals. The study was approved by the independent Ethics Committee. The development dynamics of parkinsonism syndrome of neurotoxic and neuroinflammatory genesis was assessed in the study of the motor activity of animals, as well as in the laboratory study of biomarkers of dopamine metabolism (dopamine and homovanillic acid) in blood serum and cerebrospinal fluid obtained in 7 and 21 days after the first administration of rotenone or lipopolysaccharide, and also after a single intravenous injection of allogeneic (rat) multipotent mesenchymal stromal cells (MMSC) carried out after 9 injections of rotenone. Results. A decrease in the levels of dopamine and homovanillic acid has been shown in laboratory animals on the development of Parkinson’s syndrome. In rats with a neuroinflammatory model of parkinsonism syndrome, a pre-motor stage of motor disorders development has been laboratorially confirmed. During the first weeks after the introduction of MMSC, regression of the motor symptoms of neurotoxic parkinsonism syndrome and a parallel increase in dopamine and homovanillic acid are determined. Conclusions. The effectiveness of MMSC in the early post-transplantation period is associated with the paracrine effect. It is proposed to call activated microglia, a potential therapeutic target in PD, neuroinflammatory penumbra.
实验动物帕金森综合征的形成。神经炎症半影
从实验动物的研究中获得了许多关于帕金森病(PD)发展的宝贵信息。目标。比较神经毒性和神经炎症性帕金森综合征在实验动物中的发展。材料和方法。神经炎症模型(脂多糖)组大鼠6只,神经毒性模型(鱼藤酮)组大鼠20只。对照组5只。这项研究得到了独立伦理委员会的批准。通过对动物运动活动的研究,以及在第一次给药鱼藤酮或脂多糖后7天和21天的血清和脑脊液中多巴胺代谢生物标志物(多巴胺和同型香草酸)的实验室研究,评估了神经毒性和神经炎症发生的帕金森综合征的发展动态。单次静脉注射同种异体(大鼠)多能间充质间质细胞(MMSC)后,鱼藤酮注射9次。结果。多巴胺和同型香草酸水平的下降在帕金森综合症的发展过程中已经在实验动物中得到证实。在帕金森综合征的神经炎症模型大鼠中,运动障碍发展的前运动阶段已被实验室证实。在引入MMSC后的第一周内,确定神经毒性帕金森综合征的运动症状消退,多巴胺和同型香草酸平行增加。结论。移植后早期MMSC的有效性与旁分泌作用有关。活化的小胶质细胞是帕金森病的潜在治疗靶点,我们建议将其称为神经炎性半暗带。
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