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首页> 外文期刊>International journal of molecular medicine >ATP-sensitive K+ channels contribute to the protective effects of exogenous hydrogen sulfide against high glucose-induced injury in H9c2 cardiac cells
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ATP-sensitive K+ channels contribute to the protective effects of exogenous hydrogen sulfide against high glucose-induced injury in H9c2 cardiac cells

机译:ATP敏感的K +通道有助于外源性硫化氢对高糖诱导的H9c2心肌损伤的保护作用

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摘要

Hyperglycemia, as well as diabetes mellitus, has been shown to impair ATP-sensitive K+ (K-ATP) channels in human vascular smooth muscle cells. Hydrogen sulfide (H2S) is also known to be an opener of K-ATP channels. We previously demonstrated the cardioprotective effects exerted by H2S against high-glucose (HG, 35 mM glucose)-induced injury in H9c2 cardiac cells. As such, we hypothesized that K-ATP channels play a role in the cardioprotective effects of H2S against HG-induced injury. In this study, to examine this hypothesis, H9c2 cardiac cells were treated with HG for 24 h to establish a model of HG-induced insults. Our findings revealed that treatment of the cells with HG markedly decreased the expression level of K-ATP channels. However, the decreased expression of K-ATP channels was reversed by the treatment of the cells with 400 mu M sodium hydrogen sulfide (NaHS, a donor of H2S) for 30 min prior to exposure to HG. Additionally, the HG-induced cardiomyocyte injuries, including cytotoxicity, apoptosis, oxidative stress and mitochondrial damage, were ameliorated by treatment with NaHS or 100 mu M diazoxide (a mitochondrial K-ATP channel opener) or 50 mu M pinacidil (a non-selective K-ATP channel opener) for 30 min prior to exposure to HG, as indicated by an increase in cell viability, as well as a decrease in the number of apoptotic cells, the expression of cleaved caspase-3, the generation of reactive oxygen species (ROS) and the dissipation of mitochondrial membrane potential (MMP). Notably, treatment of the H9c2 cardiac cells with 100 mu M 5-hydroxydecanoic acid (5-HD, a mitochondrial K-ATP channel blocker) or 1 mM glibenclamide (Gli, a non-selective K-ATP channel blocker) for 30 min prior to treatment with NaHS and exposure to HG significantly attenuated the above-mentioned cardioprotective effects exerted by NaHS. Notably, treatment of the cells with 500 mu M N-acetyl-L-cysteine (NAC, a scavenger of ROS) for 60 min prior to exposure to HG markedly reduced the HG-induced inhibitory effect on the expression of K-ATP channels. Taken together, our results suggest that K-ATP channels play an important role in the cardioprotective effects of exogenous H2S against HG-induced injury. This study also provides novel data demonstraring that there is an antagonistic interaction between ROS and K-ATP channels in HG-exposed H9c2 cardiac cells.
机译:高血糖症和糖尿病已经显示出会损害人血管平滑肌细胞中ATP敏感的K +(K-ATP)通道。还已知硫化氢(H2S)是K-ATP通道的开放剂。我们先前证明了H2S对H9c2心脏细胞中的高糖(HG,35 mM葡萄糖)诱导的损伤产生的心脏保护作用。因此,我们假设K-ATP通道在H2S对HG诱导的损伤的心脏保护作用中起作用。在这项研究中,为检验这一假设,将HG处理H9c2心肌细胞24小时,以建立HG诱导的损伤模型。我们的发现表明,用HG处理细胞会明显降低K-ATP通道的表达水平。然而,在暴露于HG之前,用400μM硫化氢钠(NaHS,H2S的供体)处理细胞30分钟,可以逆转K-ATP通道表达的下降。此外,通过用NaHS或100μM二氮嗪(线粒体K-ATP通道开放剂)或50μM吡那地尔(非选择性)治疗,可以缓解HG诱导的心肌细胞损伤,包括细胞毒性,凋亡,氧化应激和线粒体损伤。 K-ATP通道开放剂)暴露于HG前30分钟,这表现为细胞活力的增加以及凋亡细胞数量的减少,裂解的caspase-3的表达,活性氧的产生(ROS)和线粒体膜电位的耗散(MMP)。值得注意的是,之前用100μM 5-羟基癸酸(5-HD,线粒体K-ATP通道阻滞剂)或1 mM格列苯脲(Gli,非选择性K-ATP通道阻滞剂)治疗H9c2心脏细胞30分钟NaHS的治疗和暴露于HG会大大减弱NaHS产生的上述心脏保护作用。值得注意的是,在暴露于HG之前,用500μMN-乙酰基-L-半胱氨酸(NAC,ROS的清除剂)处理细胞60分钟,显着降低了HG诱导的对K-ATP通道表达的抑制作用。综上所述,我们的结果表明,K-ATP通道在外源H2S对HG诱导的损伤的心脏保护作用中起着重要作用。这项研究还提供了新颖的数据,证明在暴露于HG的H9c2心脏细胞中ROS和K-ATP通道之间存在拮抗作用。

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