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正常成人中枢神经系统中,小胶质细胞的局部分布差异可达一个数量级。

Local distribution of microglia in the normal adult human central nervous system differs by up to one order of magnitude.

作者信息

Mittelbronn M, Dietz K, Schluesener H J, Meyermann R

机构信息

Institute of Brain Research, University of Tuebingen, Medical School, Calwer Strasse 3, 72076 Tuebingen, Germany.

出版信息

Acta Neuropathol. 2001 Mar;101(3):249-55. doi: 10.1007/s004010000284.

Abstract

Although microglia are considered to be a sensitive sensor for pathological processes in the central nervous system, there are only a few studies about the distribution and density of microglia in the normal human brain. Therefore, a study of local density of microglial cells was conducted by investigating 20 normal human brains with no clinical neurological symptoms or diseases and no neuropathological alterations. Microglial cells were visualized by immunolabeling of proteins which are known to be expressed either constitutively or facultatively, such as CD68, major histocompatibility complex class II (MHC-II), leukocyte common antigen (LCA), leukocyte chemotactic factor (LCF), macrophage inhibitory factor-related protein (MRP) 8, MRP14, CD4 and allograft-inflammatory factor-1 (AIF-1). CD68, MHC-II and AIF-1 showed the highest densities with significant regional differences ranging from 0.5% to 16.6% of all cells in the brain parenchyma with significantly more microglia in white than in gray matter. LCF and LCA showed a similar pattern of distribution as the proteins described above, but with lower percentages of microglial cells. CD4 was not found in the brain parenchyma. We conclude that CD68, MHC-II and AIF-1 define the main microglial cell population, whereas LCF and LCA are expressed by a subpopulation of microglial cells. The brains showed no or a negligible vascular expression of MRP8 and MRP14. Information about the local microglia density in the normal human brain can serve as a reference for the evaluation of pathological microglial responses.

摘要

尽管小胶质细胞被认为是中枢神经系统病理过程的敏感传感器,但关于正常人类大脑中小胶质细胞的分布和密度的研究却很少。因此,通过研究20例无临床神经症状或疾病且无神经病理学改变的正常人类大脑,对小胶质细胞的局部密度进行了研究。通过对已知组成性或兼性表达的蛋白质进行免疫标记来观察小胶质细胞,这些蛋白质如CD68、主要组织相容性复合体II类(MHC-II)、白细胞共同抗原(LCA)、白细胞趋化因子(LCF)、巨噬细胞抑制因子相关蛋白(MRP)8、MRP14、CD4和同种异体移植炎症因子-1(AIF-1)。CD68、MHC-II和AIF-1显示出最高的密度,在脑实质中所有细胞的0.5%至16.6%之间存在显著的区域差异,白质中的小胶质细胞明显多于灰质。LCF和LCA显示出与上述蛋白质相似的分布模式,但小胶质细胞的百分比更低。在脑实质中未发现CD4。我们得出结论,CD68、MHC-II和AIF-1定义了主要的小胶质细胞群体,而LCF和LCA由小胶质细胞的一个亚群表达。这些大脑中MRP8和MRP14的血管表达无或可忽略不计。关于正常人类大脑中局部小胶质细胞密度的信息可作为评估病理性小胶质细胞反应的参考。

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