Immunological context of brain injury

Medical immunology (London, England) Pub Date : 2021-02-26 DOI:10.15789/1563-0625-ICO-2011

N. Plekhova, I. Radkov, S. Zinoviev, V. B. Shumatov

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Abstract

The parameters of several populations of immune cells (T cell populations, macrophage subpopulations) in peripheral blood and brain were studied in a clinically significant model of mild traumatic brain injury among rats. The population of resident cells of innate immunity of microglia and brain astrocytes with local tissue damage is involved in the implementation of the inflammatory response, it is also shown that in case of trauma, blood leukocytes can overcome the blood-brain barrier and penetrate the brain parenchyma. The methods of flow cytometry and immunofluorescence were used. An increase in the number of monocytes and neutrophils up to 1 day, after a mild traumatic brain injury (TBI) with a subsequent decrease to the end of the observation period was noticed. It was determined, that the number of CD45+ cells, CD3+T cells decreased at 1 days post-injury (dpi), and rose slightly by 14 dpi, the percentage of CD4+T cells continuously declined from 7 to 14 dpi, while the percentage of CD8+T cells increased from 7 to 14 dpi. With mild traumatic brain injury in animals, a significant (3-10 times) decrease in the number of microvessels with a positive reaction to the presence of SMI 71 on the 8th and 14th day after head injury was observed. Intensive staining of SMI 71 microvessels was sometimes observed with an increase in the area of a positive reaction. Thin positive deposits of the reaction product are observed in the brain of healthy animals around the wall of the microvessel. In the damaged brain, CD45high/CD11b+ positive macrophages of the M1 subpopulation appeared in the brain tissue on the 2nd day after TBI and a significant amount was observed on the 8-14th day. In the corpus callosum and ipsilateral region of the striatum, the content of cells expressing CD16/11b+ reached a maximum 8 days after TBI, which correlated with a decrease in the positive response to the presence of endothelial antigen SMI 71. Thus, in the acute period of mild TBI, the presence of neuroimmunopathological processes is determined in the brain, which can subsequently result to the dysregulation of neuroimmune connections.

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脑损伤的免疫学背景

在具有临床意义的大鼠轻度创伤性脑损伤模型中，研究了外周血和脑中几种免疫细胞群(T细胞群、巨噬细胞亚群)的参数。局部组织损伤的小胶质细胞和脑星形胶质细胞的固有免疫驻留细胞群参与了炎症反应的实施，也表明在创伤情况下，血白细胞可以克服血脑屏障并穿透脑实质。采用流式细胞术和免疫荧光法。在轻度创伤性脑损伤(TBI)后1天内，单核细胞和中性粒细胞数量增加，随后在观察期结束时下降。结果表明，CD45+细胞、CD3+T细胞数量在损伤后1天(dpi)下降，并小幅上升14 dpi, CD4+T细胞百分比从7 - 14 dpi持续下降，而CD8+T细胞百分比从7 - 14 dpi持续上升。在轻度颅脑损伤动物中，观察到SMI 71在颅脑损伤后第8天和第14天呈阳性反应的微血管数量明显减少(3-10倍)。smi71微血管的强化染色有时观察到阳性反应面积的增加。在健康动物的大脑微血管壁周围观察到薄的阳性反应产物沉积。损伤脑组织中CD45high/CD11b+阳性巨噬细胞M1亚群出现于TBI后第2天，并在第8-14天大量出现。在胼胝体和纹状体同侧区，表达CD16/11b+的细胞含量在脑损伤后8天达到最大值，这与内皮抗原SMI 71存在的阳性反应减少有关。因此，在轻度TBI的急性期，大脑中神经免疫病理过程的存在是确定的，这可能随后导致神经免疫连接的失调。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Medical immunology (London, England)

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