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Extracellular chromatin is an important mediator of ischemic stroke in mice

机译:细胞外染色质是小鼠缺血性中风的重要介质

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Objective-Recently, a growing number of studies have revealed a prothrombotic and cytotoxic role for extracellular chromatin. Cerebral ischemia/reperfusion injury is characterized by a significant amount of cell death and neutrophil activation, both of which may result in the release of chromatin. The goal of this study was to assess the effect of extracellular chromatin in ischemic stroke using a mouse model of transient middle cerebral artery occlusion. Methods and Results-Similar to reports in stroke patients, we observed increased levels of circulating nucleosomes and DNA after ischemic stroke in mice. In addition, we observed that general hypoxia also augmented extracellular chromatin. We hypothesized that targeting extracellular chromatin components would be protective in ischemic stroke. Indeed, treatment with recombinant human DNase 1 significantly improved stroke outcome. Neutralization of histones using an antihistone antibody was also protective as evidenced by smaller infarct volumes, whereas increasing levels of extracellular histones via histone infusion exacerbated stroke outcome by increasing infarct size and worsening functional outcome. Conclusion-Our results indicate that extracellular chromatin is generated and is detrimental during cerebral ischemia/reperfusion in mice. Targeting DNA and histones may be a new therapeutic strategy to limit injury resulting from ischemic stroke.
机译:目的-最近,越来越多的研究表明细胞外染色质具有促血栓形成和细胞毒性作用。脑缺血/再灌注损伤的特征在于大量的细胞死亡和中性粒细胞活化,这两者都可能导致染色质的释放。这项研究的目的是使用短暂的大脑中动脉阻塞模型来评估细胞外染色质在缺血性卒中中的作用。方法和结果-与中风患者的报道相似,我们观察到小鼠缺血性中风后循环核小体和DNA的水平增加。此外,我们观察到一般的缺氧也会增加细胞外染色质。我们假设靶向细胞外染色质成分在缺血性卒中中具有保护作用。确实,用重组人DNase 1治疗可显着改善卒中预后。如梗塞体积较小所证明,使用抗组蛋白抗体中和组蛋白也具有保护作用,而通过组蛋白输注增加的细胞外组蛋白水平则通过增加梗死面积和恶化功能预后而加重卒中预后。结论-我们的结果表明,小鼠脑缺血/再灌注过程中会产生细胞外染色质,这对细胞有害。靶向DNA和组蛋白可能是一种新的治疗策略,可以限制缺血性中风引起的损伤。

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