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正常大鼠脑中hepcidin mRNA和蛋白的表达及细胞定位

Expression and cellular localization of hepcidin mRNA and protein in normal rat brain.

作者信息

Raha-Chowdhury Ruma, Raha Animesh Alexander, Forostyak Serhiy, Zhao Jing-Wei, Stott Simon Russell William, Bomford Adrian

机构信息

John Van Geest Centre for Brain Repair, Department of Clinical Neuroscience, University of Cambridge, Cambridge, UK.

Institute of Liver Studies, King's College Hospital, London, UK.

出版信息

BMC Neurosci. 2015 Apr 21;16:24. doi: 10.1186/s12868-015-0161-7.

Abstract

BACKGROUND

Hepcidin is a peptide hormone belonging to the defensin family of cationic antimicrobial molecules that has an essential role in systemic iron homeostasis. The peptide is synthesised by hepatocytes and transported in the circulation to target tissues where it regulates the iron export function of the ferrous iron permease, ferroportin. In the brain hepcidin protein has been identified using immuno-histochemistry and mRNA by real-time PCR but not by in situ hybridisation raising the question of whether there is measurable transcription of the hepcidin gene in the central nervous system. Alternatively hepcidin could be transported as a hormone to the brain via the circulation.

RESULTS

By RT-PCR hepcidin mRNA was present at low level throughout normal rat brain while in situ hybridisation to detect low-abundant mRNA revealed that transcripts were restricted to endothelium of blood vessels and choroid plexus. In contrast, hepcidin protein analysed by immuno-histochemistry was highly expressed in blood vessels, in endothelium and in pericytes. Hepcidin was also present in glial cells and in the olfactory bulb, sub-ventricular zone and dentate gyrus, areas where neurogenesis and synaptic plasticity are maintained throughout adult life. The hepcidin species identified by Western blotting in sub-ventricular zone, cortex and hippocampus migrated as a ~2.8 kDa band, identical in size to hepcidin present in normal rat serum suggesting that hepcidin in brain was the full-length biologically active 25 amino acid peptide. Hepcidin co-localised with ferroportin in ependymal cells of the sub-ventricular zone and in the corpus callosum consistent with a regulatory role in iron metabolism at these sites.

CONCLUSIONS

Hepcidin protein was widely expressed in brain parenchyma while levels of hepcidin gene transcription appeared to be below the limits of detection of the in situ hybridisation probes. This disparity suggests that not all hepcidin in the brain is transcribed in situ and may originate in part outside the brain. The properties of hepcidin as a cationic peptide hormone are reflected in the finding of hepcidin in the walls of blood vessels and in pericytes and glia, cells that may be involved in transporting the peptide into brain interstitium.

摘要

背景

铁调素是一种属于阳离子抗菌分子防御素家族的肽激素,在全身铁稳态中起重要作用。该肽由肝细胞合成,并在循环中运输到靶组织,在那里它调节亚铁离子通透酶铁转运蛋白的铁输出功能。在大脑中,已通过免疫组织化学和实时聚合酶链反应(PCR)鉴定出铁调素蛋白,但原位杂交未检测到,这就提出了中枢神经系统中铁调素基因是否存在可测量转录的问题。另外,铁调素可能作为一种激素通过循环运输到大脑。

结果

通过逆转录PCR(RT-PCR),在正常大鼠全脑中均存在低水平的铁调素信使核糖核酸(mRNA),而用于检测低丰度mRNA的原位杂交显示,转录本仅限于血管内皮和脉络丛。相比之下,通过免疫组织化学分析的铁调素蛋白在血管、内皮细胞和周细胞中高度表达。铁调素也存在于神经胶质细胞以及嗅球、脑室下区和齿状回中,这些区域在成年期都维持着神经发生和突触可塑性。在脑室下区、皮质和海马体中通过蛋白质免疫印迹法鉴定的铁调素条带迁移为约2.8千道尔顿(kDa)的条带,其大小与正常大鼠血清中的铁调素相同,这表明大脑中的铁调素是全长具有生物活性的25个氨基酸的肽。铁调素在脑室下区的室管膜细胞和胼胝体中与铁转运蛋白共定位,这与这些部位铁代谢中的调节作用一致。

结论

铁调素蛋白在脑实质中广泛表达,而铁调素基因转录水平似乎低于原位杂交探针的检测限。这种差异表明,大脑中的铁调素并非全部在原位转录,可能部分起源于脑外。铁调素作为一种阳离子肽激素的特性体现在血管壁、周细胞和神经胶质细胞中发现铁调素,这些细胞可能参与将该肽转运到脑间质中。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f955/4409766/8d56349320c6/12868_2015_161_Fig1_HTML.jpg

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