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摘要:
The present study characterized the nerve growth factor (NGF)-mediated regulation of tau protein expression and transcription in IMR32 human neuroblastoma cells. Treatment of IMR32 cells with 50 ng/mL NGF resulted in increased levels of specific tau protein isoforms. A 550 bp fragment of the tau promoter was cloned and treatment of transfected IMR32 and PC12 cells with NGF also resulted in increased promoter activation, suggesting that the NGF-mediated increase in tau isoforms is regulated, at least in part, at the level of transcription. Pretreatment with the MAP kinase inhibitor U0126 or the PKC inhibitor bisindolylmaleimide 1 (BIS-1) attenuated the NGF-mediated increase in tau transcription, indicating that the NGF-mediated activation of the MAP kinase and PKC signaling pathways modulate tau transcription. Pre-treatment of cells with the Akt inhibitor, LY294002 or with NOS inhibitors Nω-nitro-L-arginine methylester (L-NAME) or s-methylisothiourea (S-MIU) had no effect on the NGF-mediated increase in tau promoter activation, suggesting that NO and the NGF-Akt signaling pathway do not modulate tau transcription. Taken together, these data demonstrate that NGF increases the levels of multiple human tau isoforms in IMR32 cells which may result, at least in part, from NGF-mediated PKC and MAP kinase-induced tau transcription.
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篇名 Nerve Growth Factor Enhances Tau Isoform Expression and Transcription in IMR32 Cells
来源期刊 神经系统科学与医药(英文) 学科 医学
关键词 Nerve Growth Factor (NGF) TAU Signal TRANSDUCTION Transcription NITRIC Oxide (NO) IMR32 CELLS PC12 CELLS
年,卷(期) 2014,(2) 所属期刊栏目
研究方向 页码范围 119-130
页数 12页 分类号 R73
字数 语种
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节点文献
Nerve
Growth
Factor
(NGF)
TAU
Signal
TRANSDUCTION
Transcription
NITRIC
Oxide
(NO)
IMR32
CELLS
PC12
CELLS
研究起点
研究来源
研究分支
研究去脉
引文网络交叉学科
相关学者/机构
期刊影响力
神经系统科学与医药(英文)
季刊
2158-2912
武汉市江夏区汤逊湖北路38号光谷总部空间
出版文献量(篇)
287
总下载数(次)
0
总被引数(次)
0
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