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The action of mimetic peptides on connexins protects fibroblasts from the negative effects of ischemia reperfusion

机译:模拟肽对连接蛋白的作用可保护成纤维细胞免受缺血再灌注的负面影响

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Connexins have been proposed as a target for therapeutic treatment of a variety of conditions. The main approaches have been by antisense or small peptides specific against connexins. Some of these peptides enhance communication while others interfere with connexin binding partners or bind to the intracellular and extracellular loops of connexins. Here, we explored the mechanism of action of a connexin mimetic peptide by evaluating its effect on gap junction channels, connexin protein levels and hemichannel activity in fibroblast cells under normal conditions and following ischemia reperfusion injury which elevates Cx43 levels, increases hemichannel activity and causes cell death. Our results showed that the effects of the mimetic peptide were concentration-dependent. High concentrations (100-300?μM) significantly reduced Cx43 protein levels and GJIC within 2?h, while these effects did not appear until 6?h when using lower concentrations (10-30?μM). Cell death can be reduced when hemichannel opening and GJIC were minimised.
机译:已经提出连接蛋白作为治疗各种病症的靶标。主要方法是针对连接蛋白的反义或小肽。这些肽中的一些增强了交流,而另一些则干扰了连接蛋白结合伴侣或与连接蛋白的细胞内和细胞外环结合。在这里,我们通过评估连接蛋白模拟肽对成纤维细胞在正常条件下对间隙连接通道,连接蛋白蛋白水平和半通道活性的影响以及缺血再灌注损伤(其升高Cx43水平,增加半通道活性并引起细胞)的作用来探讨其作用机制。死亡。我们的结果表明,模拟肽的作用是浓度依赖性的。高浓度(100-300μM)会在2?h内显着降低Cx43蛋白水平和GJIC,而当使用较低浓度(10-30?M)时,这些效应要等到6μh才会出现。当半通道开放和GJIC减至最小时,可以减少细胞死亡。

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