Pro-inflammatory effects of placebo neurosurgery in rats: age-related features

A. Nefodova, M. Rudyk, M. Pasichnichenko, R. Dovhyi, T. Dovbynchuk, G. Tolstanova, L. Skivka
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引用次数: 1

Abstract

Alzheimer’s disease (AD) and Parkinson’s disease (PD) are the two most prevalent neurodegenerative diseases, affecting millions of people globally and causing significant disability and mortality. Animal models are the final step in completing preclinical studies and the most appropriate approach for gaining a thorough understanding of disease pathophysiology. Modeling of idiopathic AD and PD in rodents requires stereotactic injections of disease‑triggering substances. The placebo surgery group is an integral component of the design of these experiments in order to diminish study bias as a result of animal stress and non‑specific surgical impact. Inflammation is the most commonly reported non‑specific post‑surgery phenomenon, which can manifest in different ways in animals of different ages used in these experiments. Objective — to compare the long‑term pro‑inflammatory effects of placebo surgery, commonly employed for PD and AD modeling, in rats of different ages. Materials and methods. Adult male Wistar rats aged 4 and 14 months were used in the study. The placebo surgery consisted of a stereotactic unilateral intracerebral infusion of buffer solution. Before the placebo surgery, animals were anaesthetized using ketamine or xylazine administered intraperitoneally. Intact animals of both ages were used as a control. The evaluation of pro‑inflammatory effects of placebo surgery was conducted using biomarkers of local and systemic inflammation: metabolic polarization of phagocytes (microglia, peripheral blood cells), C‑reactive protein (CRP) plasma level, and systemic inflammation indexes calculated from the hemogram study. Results. In young lesioned animals, a pronounced pro‑inflammatory functional shift of microglia and signs of the resolution of systemic inflammation (an anti‑inflammatory skew of circulating phagocyte metabolism as compared to age‑matched intact controls) were observed in the long term after the placebo neurosurgery. In old intact animals, hematological and immunological markers of low‑grade systemic inflammation were observed. In lesioned old rats, residual neuroinflammation along with pronounced systemic inflammatory responses (leukocytosis, substantially increased SIRI and SII values, pro‑inflammatory metabolic shift of peripheral blood phagocytes as compared to age‑matched intact controls) were registered. Conclusions. The effects of placebo neurosurgical manipulations in rats depend on age. Meta‑inflammation inherent to aged rats is aggravated by non‑specific post‑surgery inflammation, leading to pronounced, persistent systemic inflammatory responses.  
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大鼠神经外科安慰剂的促炎作用:与年龄相关的特征
阿尔茨海默病(AD)和帕金森病(PD)是两种最常见的神经退行性疾病,影响着全球数百万人,并造成严重的残疾和死亡。动物模型是完成临床前研究的最后一步,也是深入了解疾病病理生理的最合适方法。在啮齿类动物中建立特发性AD和PD模型需要立体定向注射疾病触发物质。安慰剂手术组是这些实验设计的一个组成部分,以减少由于动物应激和非特异性手术影响而导致的研究偏差。炎症是最常见的非特异性手术后现象,在这些实验中使用的不同年龄的动物中可以以不同的方式表现出来。目的:比较不同年龄大鼠PD和AD模型中常用的安慰剂手术的长期促炎作用。材料和方法。研究对象为4月龄和14月龄成年雄性Wistar大鼠。安慰剂手术包括立体定向单侧脑内注入缓冲溶液。在安慰剂手术之前,动物被用氯胺酮或噻嗪腹腔麻醉。两个年龄的完整动物作为对照。使用局部和全身炎症的生物标志物:吞噬细胞(小胶质细胞、外周血细胞)的代谢极化、C反应蛋白(CRP)血浆水平和血象研究计算的全身炎症指标来评估安慰剂手术的促炎作用。在年轻的病变动物中,在安慰剂神经外科手术后长期观察到小胶质细胞明显的促炎功能转移和全身炎症消退的迹象(与年龄匹配的完整对照相比,循环吞噬细胞代谢的抗炎倾斜)。在年老的完整动物中,观察到低度全身性炎症的血液学和免疫学标志物。在受损的老年大鼠中,残留的神经炎症伴随着明显的全身炎症反应(白细胞增多,SIRI和SII值显著增加,与年龄匹配的完整对照组相比,外周血吞噬细胞的促炎代谢改变)被记录下来。安慰剂神经外科操作对大鼠的影响取决于年龄。老年大鼠固有的元性炎症会因非特异性手术后炎症而加重,导致明显的、持续的全身炎症反应。
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