Nrf2 attenuates methamphetamine-induced myocardial injury by regulating oxidative stress and apoptosis in mice.

Hao Yu, Yanxia Peng, Wenjuan Dong, Baoyu Shen, Genmeng Yang, Qianyun Nie, Yan Tian, Lixiang Qin, Chunhui Song, Bingzheng Chen, Yongna Zhao, Lihua Li, Shijun Hong
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Abstract

Objectives: Methamphetamine (MA) abuse is a serious social problem worldwide. Cardiovascular complications were the second leading cause of death among MA abusers. We aimed to clarify the effects of MA on myocardial injury, oxidative stress, and apoptosis in myocardial cells and to explore the potential mechanism of nuclear factor-erythroid factor 2-related factor 2 (Nrf2) in MA-induced oxidative stress and apoptosis.

Methods: An acute cardiac toxicity model of MA was established by intraperitoneal injection of MA (2 mg/kg) for 5 days. Nrf2 activation (by sulforaphane (SFN) 1 h before MA injection) and Nrf2 gene knockout were performed to explore the regulatory effects of Nrf2 on cardiac toxicity.

Results: The protein expressions of Nrf2 (p < .001) and heme oxygenase-1 (HO-1) were increased (p < .01), suggesting that MA activated the Nrf2/HO-1 pathway. In the MA group, cardiac injury score (p < .001) and cardiac troponin I (cTnI) protein expression increased (p < .01). Malondialdehyde (MDA) content increased (p < .001), superoxide dismutase (SOD) activity decreased (p < .05). Protein expressions of Caspase-3 (p < .001) and Bax (p < .001) increased, and Bcl-2 decreased (p < .001) as well. These changes were reversed by activation of Nrf2 but became more pronounced after Nrf2 knockout, suggested that the activation and knockout of Nrf2 attenuated and aggravated MA-induced myocardial injury, oxidative stress and apoptosis in myocardial cells, respectively.

Conclusions: MA administration induced myocardial injury, oxidative stress, and apoptosis in mice. Nrf2 attenuated MA-induced myocardial injury by regulating oxidative stress and apoptosis, thus playing a protective role.

Nrf2通过调节氧化应激和细胞凋亡减轻甲基苯丙胺诱导的小鼠心肌损伤。
目的:甲基苯丙胺(MA)滥用是世界范围内一个严重的社会问题。心血管并发症是MA滥用者死亡的第二大原因。我们旨在阐明MA对心肌损伤、氧化应激和心肌细胞凋亡的影响,并探讨核因子-红细胞因子2相关因子2 (Nrf2)在MA诱导的氧化应激和凋亡中的潜在机制。方法:通过腹腔注射MA (2 mg/kg) 5 d建立MA急性心脏毒性模型。通过激活Nrf2 (MA注射前1 h通过萝卜硫素(SFN))和敲除Nrf2基因,探讨Nrf2对心脏毒性的调节作用。结果:Nrf2蛋白表达(p < 0.001)和血红素加氧酶-1 (HO-1)蛋白表达升高(p < 0.01),提示MA激活了Nrf2/HO-1通路。MA组心肌损伤评分(p < 0.001)和心肌肌钙蛋白I (cTnI)蛋白表达升高(p < 0.01)。丙二醛(MDA)含量升高(p < 0.001),超氧化物歧化酶(SOD)活性降低(p < 0.05)。Caspase-3 (p < 0.001)和Bax (p < 0.001)蛋白表达升高,Bcl-2蛋白表达降低(p < 0.001)。这些变化被Nrf2激活逆转,但在Nrf2敲除后变得更加明显,这表明Nrf2的激活和敲除分别减轻和加重了ma诱导的心肌损伤、氧化应激和心肌细胞凋亡。结论:MA可诱导小鼠心肌损伤、氧化应激和细胞凋亡。Nrf2通过调节氧化应激和细胞凋亡来减轻ma诱导的心肌损伤,发挥保护作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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