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X-Ray Fluorescence Imaging: A New Tool for Studying Manganese Neurotoxicity

机译:X射线荧光成像:一种新的工具研究锰的神经毒性

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摘要

The neurotoxic effect of manganese (Mn) establishes itself in a condition known as manganism or Mn induced parkinsonism. While this condition was first diagnosed about 170 years ago, the mechanism of the neurotoxic action of Mn remains unknown. Moreover, the possibility that Mn exposure combined with other genetic and environmental factors can contribute to the development of Parkinson's disease has been discussed in the literature and several epidemiological studies have demonstrated a correlation between Mn exposure and an elevated risk of Parkinson's disease. Here, we introduce X-ray fluorescence imaging as a new quantitative tool for analysis of the Mn distribution in the brain with high spatial resolution. The animal model employed mimics deficits observed in affected human subjects. The obtained maps of Mn distribution in the brain demonstrate the highest Mn content in the globus pallidus, the thalamus, and the substantia nigra pars compacta. To test the hypothesis that Mn transport into/distribution within brain cells mimics that of other biologically relevant metal ions, such as iron, copper, or zinc, their distributions were compared. It was demonstrated that the Mn distribution does not follow the distributions of any of these metals in the brain. The majority of Mn in the brain was shown to occur in the mobile state, confirming the relevance of the chelation therapy currently used to treat Mn intoxication. In cells with accumulated Mn, it can cause neurotoxic action by affecting the mitochondrial respiratory chain. This can result in increased susceptibility of the neurons of the globus pallidus, thalamus, and substantia nigra pars compacta to various environmental or genetic insults. The obtained data is the first demonstration of Mn accumulation in the substantia nigra pars compacta, and thus, can represent a link between Mn exposure and its potential effects for development of Parkinson's disease.
机译:锰(Mn)的神经毒性作用可在锰或Mn诱发的帕金森综合症中确立。尽管大约170年前首次诊断出这种疾病,但Mn的神经毒性作用机制仍不清楚。此外,文献中已经讨论了锰暴露与其他遗传和环境因素相结合可能有助于帕金森氏病发展的可能性,一些流行病学研究表明锰暴露与帕金森氏病风险升高之间存在相关性。在这里,我们介绍X射线荧光成像作为一种新的定量工具,用于以高空间分辨率分析大脑中Mn的分布。使用的动物模型模仿了在受影响的人类受试者中观察到的缺陷。获得的大脑中锰分布图表明,苍白球,丘脑和黑质致密物中的锰含量最高。为了检验这样的假设,即锰在脑细胞中的迁移/分布模拟了其他生物学相关的金属离子,例如铁,铜或锌,对它们的分布进行了比较。事实证明,锰的分布不符合这些金属在大脑中的分布。大脑中大部分Mn以流动状态显示,这证实了目前用于治疗Mn中毒的螯合疗法的相关性。在积累了锰的细胞中,它可以通过影响线粒体呼吸链而引起神经毒性作用。这可能导致苍白球,丘脑和黑质致密部神经元对各种环境或遗传损伤的敏感性增加。获得的数据是黑质致密部中Mn积累的首次证明,因此可以代表Mn暴露与其对帕金森氏病发展的潜在影响之间的联系。

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