Laboratory of Inflammation and Nervous System Diseases, Department of Neuroscience, Mario Negri Institute for Pharmacological Research, Milan, Italy.
J Neuroinflammation. 2011 Dec 10;8:174. doi: 10.1186/1742-2094-8-174.
Emerging evidence indicates that, similarly to what happens for peripheral macrophages, microglia can express different phenotypes depending on microenvironmental signals. In spite of the large literature on inflammation after ischemia, information on M/M phenotype marker expression, their colocalization and temporal evolution in the injured brain is lacking. The present study investigates the presence of microglia/macrophage phenotype markers, their temporal expression, whether they are concomitantly expressed by the same subpopulation, or they are expressed at distinct phases or locations in relation to the ischemic lesion.
Volume of ischemic lesion, neuronal counts and TUNEL staining were assessed in C57Bl/6 mice at 6-12-24-48 h and 7d after permanent occlusion of the middle cerebral artery. At the same time points, the expression, distribution in the lesioned area, association with a definite morphology and coexpression of the microglia/macrophage markers CD11b, CD45, CD68, Ym1, CD206 were assessed by immunostaining and confocal microscopy.
The results show that: 1) the ischemic lesion induces the expression of selected microglia/macrophage markers that develop over time, each with a specific pattern; 2) each marker has a given localization in the lesioned area with no apparent changes during time, with the exception of CD68 that is confined in the border zone of the lesion at early times but it greatly increases and invades the ischemic core at 7d; 3) while CD68 is expressed in both ramified and globular CD11b cells, Ym1 and CD206 are exclusively expressed by globular CD11b cells.
These data show that the ischemic lesion is accompanied by activation of specific microglia/macrophage phenotype that presents distinctive spatial and temporal features. These different states of microglia/macrophages reflect the complexity of these cells and their ability to differentiate towards a multitude of phenotypes depending on the surrounding micro-environmental signals that can change over time. The data presented in this study provide a basis for understanding this complex response and for developing strategies resulting in promotion of a protective inflammatory phenotype.
新出现的证据表明,类似于周围巨噬细胞的情况,小胶质细胞可以根据微环境信号表达不同的表型。尽管关于缺血后炎症的文献很多,但关于损伤大脑中小胶质细胞/巨噬细胞表型标志物的表达、它们的共定位以及时间演变的信息却缺乏。本研究调查了小胶质细胞/巨噬细胞表型标志物的存在、它们的时间表达,以及它们是否由同一亚群同时表达,或者它们是否在与缺血性损伤相关的不同阶段或位置表达。
在 C57Bl/6 小鼠永久性大脑中动脉闭塞后 6、12、24、48 h 和 7d 时,评估缺血性损伤体积、神经元计数和 TUNEL 染色。在相同的时间点,通过免疫染色和共聚焦显微镜评估小胶质细胞/巨噬细胞标志物 CD11b、CD45、CD68、Ym1、CD206 的表达、在损伤区域的分布、与特定形态的关联以及共表达。
结果表明:1)缺血性损伤诱导选定的小胶质细胞/巨噬细胞标志物的表达,这些标志物随时间发展,每种标志物都有特定的模式;2)每个标志物在损伤区域都有特定的定位,在时间上没有明显变化,除了 CD68,它在早期局限于损伤的边界区,但在 7d 时它大大增加并侵入缺血核心;3)虽然 CD68 表达在分支状和球状 CD11b 细胞中,但 Ym1 和 CD206 仅表达在球状 CD11b 细胞中。
这些数据表明,缺血性损伤伴随着特定的小胶质细胞/巨噬细胞表型的激活,呈现出独特的空间和时间特征。这些不同的小胶质细胞/巨噬细胞状态反映了这些细胞的复杂性及其根据周围微环境信号分化为多种表型的能力,这些信号会随时间变化。本研究中提供的数据为理解这种复杂反应和制定促进保护性炎症表型的策略提供了基础。
Zotero 插件
