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自溶以不同的速率影响人脑神经元和神经胶质细胞中铁蛋白的铁载量。

Autolysis Affects the Iron Cargo of Ferritins in Neurons and Glial Cells at Different Rates in the Human Brain.

机构信息

Gottfried Schatz Research Center, Division of Cell Biology, Histology and Embryology, Research Unit Electron Microscopic Techniques, Medical University of Graz, 8010, Graz, Austria.

Faculty of Medicine, University of Maribor, 2000, Maribor, Slovenia.

出版信息

Cell Mol Neurobiol. 2023 Aug;43(6):2909-2923. doi: 10.1007/s10571-023-01332-w. Epub 2023 Mar 15.

Abstract

Iron is known to accumulate in neurological disorders, so a careful balance of the iron concentration is essential for healthy brain functioning. An imbalance in iron homeostasis could arise due to the dysfunction of proteins involved in iron homeostasis. Here, we focus on ferritin-the primary iron storage protein of the brain. In this study, we aimed to improve a method to measure ferritin-bound iron in the human post-mortem brain, and to discern its distribution in particular cell types and brain regions. Though it is known that glial cells and neurons differ in their ferritin concentration, the change in the number and distribution of iron-filled ferritin cores between different cell types during autolysis has not been revealed yet. Here, we show the cellular and region-wide distribution of ferritin in the human brain using state-of-the-art analytical electron microscopy. We validated the concentration of iron-filled ferritin cores to the absolute iron concentration measured by quantitative MRI and inductively coupled plasma mass spectrometry. We show that ferritins lose iron from their cores with the progression of autolysis whereas the overall iron concentrations were unaffected. Although the highest concentration of ferritin was found in glial cells, as the total ferritin concentration increased in a patient, ferritin accumulated more in neurons than in glial cells. Summed up, our findings point out the unique behaviour of neurons in storing iron during autolysis and explain the differences between the absolute iron concentrations and iron-filled ferritin in a cell-type-dependent manner in the human brain. The rate of loss of the iron-filled ferritin cores during autolysis is higher in neurons than in glial cells.

摘要

铁已知在神经紊乱中积累,因此健康大脑功能对铁浓度的精细平衡至关重要。铁稳态的失衡可能由于涉及铁稳态的蛋白质功能障碍而出现。在这里,我们重点关注脑内主要铁储存蛋白-铁蛋白。在这项研究中,我们旨在改进一种测量人死后脑中铁蛋白结合铁的方法,并辨别其在特定细胞类型和脑区的分布。虽然已知神经胶质细胞和神经元在铁蛋白浓度上存在差异,但在自溶过程中不同细胞类型之间铁填充铁蛋白核心的数量和分布的变化尚未被揭示。在这里,我们使用最先进的分析电子显微镜展示了人脑中铁蛋白的细胞和全脑分布。我们通过定量 MRI 和电感耦合等离子体质谱验证了铁填充铁蛋白核心的浓度与绝对铁浓度。我们表明,铁蛋白随着自溶的进行从核心中失去铁,而总铁浓度不受影响。尽管铁蛋白的最高浓度存在于神经胶质细胞中,但随着患者中总铁蛋白浓度的增加,铁蛋白在神经元中的积累多于在神经胶质细胞中。总之,我们的研究结果指出了神经元在自溶过程中储存铁的独特行为,并以细胞类型依赖的方式解释了人脑内绝对铁浓度和铁填充铁蛋白之间的差异。在自溶过程中铁填充铁蛋白核心的丢失率在神经元中高于神经胶质细胞。

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