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PC12 分化为神经元后细胞内铜浓度和铜调节基因表达的变化。

Changes in intracellular copper concentration and copper-regulating gene expression after PC12 differentiation into neurons.

机构信息

Laboratory of Toxicology and Environmental Health, Graduate School of Pharmaceutical Sciences, Chiba University, Chuo, Chiba 260-8675, Japan.

Laboratory of Chemical Toxicology and Environmental Health, Showa Pharmaceutical University, Machida, Tokyo 194-8543, Japan.

出版信息

Sci Rep. 2016 Sep 13;6:33007. doi: 10.1038/srep33007.

Abstract

It is suspected that some neurodegenerative diseases are a result of the disturbance of copper (Cu) homeostasis, although it remains unclear whether the disturbance of Cu homeostasis has aberrant effects on neurons. Herein, we investigated Cu metabolism specifically in neurons in terms of changes in the intracellular Cu concentration and the expression of Cu-regulating genes, such as Cu transporters and metallothioneins (MTs), before and after the differentiation of rat pheochromocytoma cells (PC12 cells) into neurons. After the differentiation, Cu and Zn imaging with fluorescent probes revealed an increase in intracellular Cu concentration. The concentrations of other essential metals, which were determined by an inductively coupled plasma mass spectrometer, were not altered. The mRNA expression of the Cu influx transporter, Ctr1, was decreased after the differentiation, and the differentiated cells acquired tolerance to Cu and cisplatin, another substrate of Ctr1. In addition, the expression of MT-3, a brain-specific isoform, was increased, contrary to the decreased expression of MT-1 and MT-2. Taken together, the differentiation of PC12 cells into neurons induced MT-3 expression, thereby resulting in intracellular Cu accumulation. The decrease in Ctr1 expression was assumed to be a response aimed at abolishing the physiological accumulation of Cu after the differentiation.

摘要

据推测,一些神经退行性疾病是铜(Cu)稳态失调的结果,尽管尚不清楚 Cu 稳态失调是否对神经元产生异常影响。在此,我们研究了大鼠嗜铬细胞瘤细胞(PC12 细胞)分化为神经元前后,神经元内 Cu 代谢的变化,包括细胞内 Cu 浓度和 Cu 调节基因(如 Cu 转运体和金属硫蛋白(MTs))的表达变化。分化后,用荧光探针进行 Cu 和 Zn 成像显示细胞内 Cu 浓度增加。电感耦合等离子体质谱仪测定的其他必需金属的浓度没有改变。Cu 内流转运体 Ctr1 的 mRNA 表达在分化后下降,分化后的细胞对 Cu 和顺铂(Ctr1 的另一种底物)产生了耐受性。此外,脑特异性同工型 MT-3 的表达增加,而 MT-1 和 MT-2 的表达下降。综上所述,PC12 细胞分化为神经元诱导了 MT-3 的表达,从而导致细胞内 Cu 积累。Ctr1 表达的下降被认为是分化后消除生理 Cu 积累的一种反应。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/35d6/5020689/7fff60e6061c/srep33007-f1.jpg

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