Edaravone protects against glutamate-induced PERK/EIF2¦Á/ATF4 integrated stress response and activation of caspase-12

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• 作者：Jin Fan¹ ; Hao Long¹ ; Yiming Li ; Yuwen Liu ; Wei Zhou ; Qingqing Li ; Guoyong Yin ; ^{guoyong_yin2005nanjing@yahoo.com} ; Ning Zhang ; Weihua Cai ; ^{caiwhspine@sina.com}
• 关键词：Edaravone ; Apoptosis ; PERK ; EIF2¦Á ; ATF4 ; Caspase-12
• 刊名：Brain Research
• 出版年：2013
• 出版时间：26 June, 2013
• 年：2013
• 卷：1519
• 期：Complete
• 页码：1-8
• 全文大小：3046 K

文摘

As a potent novel free radical scavenger, edaravone has been reported to have neuroprotective effects in both animals and humans, although the underlying mechanisms remain unclear. In our study, we generated a culture of almost pure neurons, which were either left untreated or prophylactically treated with edaravone, then exposed to 50 ¦ÌM glutamate for 10 min. Flow Cytometry analysis was performed to quantify the percentage of apoptotic cells. Ultrastructural changes in the endoplasmic reticulum were observed by electron microscopy. Immunofluorescence and western blotting for activation of selected related molecules, including PERK (pancreatic ER stress kinase, PERK), eIF2¦Á (eukaryotic initiation factor 2 alpha, eIF2¦Á), activating ATF4 (transcription factor 4, ATF4), and caspase-12 were examined. In Glutamate-treated group, the sequential activation of PERK, eIF2¦Á, ATF4 and caspase-12 could be observed at 2 h, and peaked at 24 h. However, treatment with edaravone was able to prevent these changes. In addition, the morphology of the endoplasmic reticulum was better preserved and the percentage of apoptotic cells was lower in cells treated with edaravone. In summary, our results indicate that ISR (PERK/eIF2/ATF4 integrated stress response, ISR) plays an important role in glutamate-induced nerve cells death, and that edaravone could protect neurons against glutamate-induced endoplasmic reticulum stress.