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首页> 外文期刊>Journal of pineal research >Enhancement of high glucose‐induced PINK1 expression by melatonin stimulates neuronal cell survival: Involvement of MT 2 2 /Akt/NF‐κB pathway
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Enhancement of high glucose‐induced PINK1 expression by melatonin stimulates neuronal cell survival: Involvement of MT 2 2 /Akt/NF‐κB pathway

机译:褪黑激素的高葡萄糖诱导的粉红色1表达的增强刺激神经元细胞存活:MT 2 2 / AKT / NF-κB途径的参与

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Abstract Hyperglycemia is a representative hallmark and risk factor for diabetes mellitus (DM) and is closely linked to DM‐associated neuronal cell death. Previous investigators reported on a genome‐wide association study and showed relationships between DM and melatonin receptor (MT), highlighting the role of MT signaling by assessing melatonin in DM. However, the role of MT signaling in DM pathogenesis is unclear. Therefore, we investigated the role of mitophagy regulators in high glucose‐induced neuronal cell death and the effect of melatonin against high glucose‐induced mitophagy regulators in neuronal cells. In our results, high glucose significantly increased PTEN‐induced putative kinase 1 (PINK1) and LC‐3B expressions; as well it decreased cytochrome c oxidase subunit 4 expression and Mitotracker? fluorescence intensity. Silencing of PINK1 induced mitochondrial reactive oxygen species (ROS) accumulation and mitochondrial membrane potential impairment, increased expressions of cleaved caspases, and increased the number of annexin V‐positive cells. In addition, high glucose‐stimulated melatonin receptor 1B ( MTNR1B ) mRNA and PINK1 expressions were reversed by ROS scavenger N ‐acetyl cysteine pretreatment. Upregulation of PINK1 expression in neuronal cells is suppressed by pretreatment with MT 2 receptor‐specific inhibitor 4‐P‐PDOT. We further showed melatonin stimulated Akt phosphorylation, which was followed by nuclear factor kappa‐light‐chain‐enhancer of activated B cells (NF‐κB) phosphorylation and nuclear translocation. Silencing of PINK1 expression abolished melatonin‐regulated mitochondrial ROS production, cleaved caspase‐3 and caspase‐9 expressions, and the number of annexin V‐positive cells. In conclusion, we have demonstrated the melatonin stimulates PINK1 expression via an MT 2 /Akt/NF‐κB pathway, and such stimulation is important for the prevention of neuronal cell apoptosis under high glucose conditions.
机译:摘要高血糖是糖尿病(DM)的代表性标志性和危险因素,并且与DM相关神经细胞死亡密切相关。先前的研究人员报告了基因组 - 宽的协会研究,并显示了DM和褪黑激素受体(MT)之间的关系,突出了MT信号传导在DM中的褪黑激素的作用。然而,MT信号传导在DM发病机制中的作用尚不清楚。因此,我们调查了MICOCHAGY调节剂在高葡萄糖诱导的神经元细胞死亡中的作用以及褪黑素对神经元细胞中的高葡萄糖诱导的MITOCHAGY调节剂的作用。在我们的结果中,高葡萄糖显着增加了PTEN诱导的推定激酶1(PINK1)和LC-3B表达;也降低了细胞色素C氧化酶亚基4表达和Mitotracker?荧光强度。粉红色的诱导的线粒体反应性氧物质(ROS)积聚和线粒体膜电位损伤,裂解胱天蛋白酶的表达增加,增加了膜蛋白V阳性细胞的数量。此外,通过ROS清除剂N-乙酰半胱氨酸预处理反转高葡萄糖刺激的褪黑激素受体1B(MTNR1B)mRNA和PINK1表达。通过用MT 2受体特异性抑制剂4-P-PPOT预处理抑制了神经元细胞中Pink1表达的上调。我们进一步展示了褪黑激素刺激的AKT磷酸化,其次是活化B细胞(NF-κB)磷酸化和核易位的核因子κ-轻链增强剂。粉红色1表达的沉默废除了褪黑激素调节的线粒体ROS生产,切割的Caspase-3和Caspase-9表达,以及膜蛋白V阳性细胞的数量。总之,我们已经证明了褪黑激素刺激Pink1的表达,通过MT 2 / Akt / NF-κB途径,这种刺激对于在高葡萄糖条件下预防神经元细胞凋亡是重要的。

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