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出生后大鼠脑中铁蛋白亚基的细胞分布

Cellular distribution of ferritin subunits in postnatal rat brain.

作者信息

Cheepsunthorn P, Palmer C, Connor J R

机构信息

Department of Neuroscience and Anatomy, M.S. Hershey Medical Center, Pennsylvania State University College of Medicine, Hershey 17033, USA.

出版信息

J Comp Neurol. 1998 Oct 12;400(1):73-86.

PMID:9762867
Abstract

The normal development of the brain requires finely coordinated events, many of which require iron. Consequently, iron must be available to the brain in a timely manner and in a bioavailable form. However, the brain also requires stringent mechanisms to protect itself from iron-induced oxidative damage. The protein that is best suited to making iron available but also adequately protecting the cell is the intracellular iron storage protein ferritin. Typically, ferritin is composed of 24 subunits of H and L chains, which are functionally distinct. This study was undertaken to determine the expression of ferritin subunits during normal development of the postnatal rat brain. There is a shift in ferritin-containing cell types during development from predominantly microglia at postnatal day 5 (PND 5) to predominantly oligodendrocytes by PND 30. At PND 5, microglia are found throughout gray and white matter areas of the brain, but only amoeboid microglia in discrete foci in the subcortical white matter are ferritin positive. At PND 15, some oligodendrocytes in the subcortical white matter express ferritin, but the majority of ferritin-containing cells within white matter are still microglia. By PND 30, the predominant ferritin-containing cell type within white matter are oligodendrocytes. Generally, the cellular distribution of both ferritin subunits were identical with one major exception; H-ferritin, but not L-ferritin, was present in neuronal nuclei in the cortex. These data suggest that microglia play a role in brain iron homeostasis during normal postnatal development and may influence myelination by competing with oligodendrocytes for iron.

摘要

大脑的正常发育需要精细协调的一系列事件,其中许多事件都需要铁元素。因此,铁必须及时且以生物可利用的形式供应给大脑。然而,大脑也需要严格的机制来保护自身免受铁诱导的氧化损伤。最适合使铁元素可利用同时又能充分保护细胞的蛋白质是细胞内铁储存蛋白铁蛋白。通常,铁蛋白由24个H链和L链亚基组成,它们在功能上有所不同。本研究旨在确定出生后大鼠大脑正常发育过程中铁蛋白亚基的表达情况。在发育过程中,含铁蛋白的细胞类型发生了转变,从出生后第5天(PND 5)主要是小胶质细胞,到PND 30时主要是少突胶质细胞。在PND 5时,小胶质细胞遍布大脑的灰质和白质区域,但只有皮质下白质中离散病灶处的阿米巴样小胶质细胞是铁蛋白阳性。在PND 15时,皮质下白质中的一些少突胶质细胞表达铁蛋白,但白质中大多数含铁蛋白的细胞仍然是小胶质细胞。到PND 30时,白质中主要的含铁蛋白细胞类型是少突胶质细胞。一般来说,两种铁蛋白亚基的细胞分布是相同的,但有一个主要例外;H-铁蛋白而非L-铁蛋白存在于皮质的神经元细胞核中。这些数据表明,小胶质细胞在出生后正常发育过程中对大脑铁稳态起作用,并且可能通过与少突胶质细胞竞争铁元素来影响髓鞘形成。

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