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小胶质细胞对原发性脱髓鞘的募集、激活和增殖。

Microglial recruitment, activation, and proliferation in response to primary demyelination.

作者信息

Remington Leah T, Babcock Alicia A, Zehntner Simone P, Owens Trevor

机构信息

Montreal Neurological Institute, McGill University, Montreal, Canada.

出版信息

Am J Pathol. 2007 May;170(5):1713-24. doi: 10.2353/ajpath.2007.060783.

Abstract

We have characterized the cellular response to demyelination/remyelination in the central nervous system using the toxin cuprizone, which causes reproducible demyelination in the corpus callosum. Microglia were distinguished from macrophages by relative CD45 expression (CD45(dim)) using flow cytometry. Their expansion occurred rapidly and substantially outnumbered infiltrating macrophages and T cells throughout the course of cuprizone treatment. We used bromodeoxyuridine incorporation and bone marrow chimeras to show that both proliferation and immigration from blood accounted for increased microglial numbers. Microglia adopted an activated phenotype during demyelination, up-regulating major histocompatibility class I and B7.2/CD86. A subpopulation of CD45(dim-high) microglia that expressed reduced levels of CD11b emerged during demyelination. These microglia expressed CD11c and were potent antigen-presenting cells in vitro. T cells were recruited to the demyelinated corpus callosum but did not appear to be activated. Our study highlights the role of microglia as a heterogeneous population of cells in primary demyelination, with the capacity to present antigen, proliferate, and migrate into demyelinated areas.

摘要

我们利用毒素铜螯合剂(cuprizone)对中枢神经系统中脱髓鞘/再髓鞘化的细胞反应进行了表征,该毒素可在胼胝体中引起可重复性脱髓鞘。通过流式细胞术利用相对CD45表达(CD45(dim))将小胶质细胞与巨噬细胞区分开来。在整个铜螯合剂治疗过程中,它们迅速扩增,数量大大超过浸润的巨噬细胞和T细胞。我们使用溴脱氧尿苷掺入法和骨髓嵌合体来表明增殖和从血液中的迁移都导致了小胶质细胞数量的增加。在脱髓鞘过程中,小胶质细胞呈现出活化表型,上调主要组织相容性复合体I类和B7.2/CD86。在脱髓鞘过程中出现了一群CD45(dim-high)小胶质细胞,其CD11b表达水平降低。这些小胶质细胞表达CD11c,在体外是有效的抗原呈递细胞。T细胞被募集到脱髓鞘的胼胝体,但似乎未被激活。我们的研究强调了小胶质细胞作为原发性脱髓鞘中异质性细胞群体的作用,具有呈递抗原、增殖和迁移到脱髓鞘区域的能力。

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