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Brain iron metabolism and its perturbation in neurological diseases

机译:脑铁代谢及其在神经系统疾病中的扰动

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Metal ions are of particular importance in brain function, notably iron. A broad overview of iron metabolism and its homeostasis both at the cellular level (involving regulation at the level of mRNA translation) and the systemic level (involving the peptide ‘hormone’ hepcidin) is presented. The mechanisms of iron transport both across the blood–brain barrier and within the brain are then examined. The importance of iron in the developing foetus and in early life is underlined. We then review the growing corpus of evidence that many neurodegenerative diseases (NDs) are the consequence of dysregulation of brain iron homeostasis. This results in the production of reactive oxygen species, generating reactive aldehydes, which, together with further oxidative insults, causes oxidative modification of proteins, manifested by carbonyl formation. These misfolded and damaged proteins overwhelm the ubiquitin/proteasome system, accumulating the characteristic inclusion bodies found in many NDs. The involvement of iron in Alzheimer’s disease and Parkinson’s disease is then examined, with emphasis on recent data linking in particular interactions between iron homeostasis and key disease proteins. We conclude that there is overwhelming evidence for a direct involvement of iron in NDs.
机译:金属离子在脑功能中尤其重要,尤其是铁。介绍了铁代谢及其在细胞水平(在mRNA翻译水平涉及调控)和系统水平(在肽“激素”铁调素中涉及)的体内稳态的概貌。然后研究了铁穿过血脑屏障和大脑内部的运输机制。强调了铁在发育中的胎儿和早期生命中的重要性。然后,我们回顾了越来越多的证据,表明许多神经退行性疾病(NDs)是脑铁稳态失调的结果。这导致产生活性氧,产生活性醛,其与进一步的氧化损伤一起导致蛋白质的氧化修饰,表现为羰基形成。这些错误折叠和损坏的蛋白质使泛素/蛋白酶体系统不堪重负,从而积聚了许多ND中发现的特征性包涵体。然后检查了铁与阿尔茨海默氏病和帕金森氏病的关系,重点是最近的数据,特别是铁稳态与关键疾病蛋白之间的相互作用。我们得出结论,有大量证据表明铁直接参与了ND。

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