外伤性脑损伤非特异性炎症反应的全身效应。

S V Ziablitsev, S V Pishchulina, S V Kolesnikova, R N Boris
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引用次数: 4

摘要

目的:探讨炎症在重型颅脑损伤所致创伤性脑疾病中的全身性作用。这项研究是在65只纯种雄性大鼠身上进行的。创伤性脑损伤(TBI)以0.52 j的能量对动物颅弓进行一次打击,伤后5天内死亡率为87%。实验动物有严重的闭合性脑外伤。研究血液循环免疫复合物、c反应蛋白、铜蓝蛋白、促炎白介素(IL-1b、IL-6、IL-8和肿瘤坏死因子a - tnf -a)的含量。循环免疫复合物水平在24小时内升高3.1倍,在伤后第5天升高4.4倍,反映出损伤动物脑组织和血液中代谢物和毒素的逐渐积累。各观察期血c反应蛋白水平均明显升高,3小时内升高3.5倍,第5天后升高21.3倍。因此,研究结果表明,全身性炎症的急性期始于创伤后第1天结束,并在创伤性脑病的病程中不断发展。血液中IL-1b含量持续升高:3小时4.7倍;24小时7.6次;伤后第5天17.4次。其他白细胞介素水平也升高,但程度较轻。循环免疫复合物、急性期蛋白和白细胞介素水平变化的一致性表明创伤性脑损伤急性期创伤性疾病的一种致病模式:损伤过程的扩散涉及身体器官和组织,并从创伤后第2天开始建立全身性炎症反应阶段。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Systemic effects of unspecific inflammatory reaction at traumatic brain injury.

To determine the role of systemic effects of inflammation at traumatic brain disease caused by severe traumatic brain injury. The study is performed on 65 white outbred male rats. TBI is applied with one blow on animal’s cranial vaults with blow energy of 0.52 J. The rate of mortality within the first 5 days after the injury is 87%. Experimental animals have got severe closed TBI. Blood contents of circulating immune complexes, C-reactive protein, ceruloplasmin, proinflammatory - interleukins(IL-1b, IL-6, IL-8 and tumor necrosis factor a -TNF-a) are investigated. The circulating immune complexes levels are increased 3.1 times in 24 hours and 4.4 times on the 5th days of trauma reflecting the progressive accumulation of metabolites and toxins in brain tissue and in the blood of injured animals. Blood levels of C-reactive protein are markedly increased in all periods of observation exceeding the control levels 3.5 times in 3 hours and 21.3 times after 5th day of trauma. Thus the study results suggest that the acute phase of systemic inflammation sets at the end of the 1st day after the trauma and it progresses in the course of traumatic brain disease. Blood contents of IL-1b increases continuously: 4.7 times in 3 hours; 7.6 times in 24 hours; and 17.4 times on the 5th day after trauma. The other interleukins levels are also increased but to a lesser extent. The coherence of changes in levels of circulating immune complexes, acute-phase proteins and interleukins indicates a pathogenic pattern of the acute period of traumatic disease at traumatic brain injury: spreading of damage processes with the involvement of body organs and tissues and the establishment of a systemic inflammatory reaction stage from the second day of posttraumatic period.

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