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Reactive Oxygen Species in Mesenchymal Stem Cell Aging: Implication to Lung Diseases

机译:间充质干细胞衰老中的活性氧:对肺部疾病的影响

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MSCs have become an emerging cell source with their immune modulation, high proliferation rate, and differentiation potential; indeed, they have been challenged in clinical trials. Recently, it has shown that ROS play a dual role as both deleterious and beneficial species depending on their concentration in MSCs. Various environmental stresses-induced excessive production of ROS triggers cellular senescence and abnormal differentiation on MSCs. Moreover, MSCs have been suggested to participate in the treatment of ALI/ARDS and COPD as a major cause of high morbidity and mortality. Therapeutic mechanisms of MSCs in the treatment of ARDS/COPD were focused on cell engraftment and paracrine action. However, ROS-mediated therapeutic mechanisms of MSCs still remain largely unknown. Here, we review the key factors associated with cell cycle and chromatin remodeling to accelerate or delay the MSC aging process. In addition, the enhanced ROS production and its associated pathophysiological pathways will be discussed along with the MSC senescence process. Furthermore, the present review highlights how the excessive amount of ROS-mediated oxidative stress might interfere with homeostasis of lungs and residual lung cells in the pathogenesis of ALI/ARDS and COPD.
机译:MSC凭借其免疫调节,高增殖率和分化潜力已成为新兴的细胞来源。实际上,它们在临床试验中受到了挑战。最近,已经表明,ROS在有害物质和有益物质中都起着双重作用,这取决于它们在MSC中的浓度。各种环境压力导致的ROS过量产生会触发MSC的细胞衰老和异常分化。此外,已经建议MSC参与ALI / ARDS和COPD的治疗,这是高发病率和死亡率的主要原因。 MSC在ARDS / COPD治疗中的治疗机制集中在细胞植入和旁分泌作用上。然而,ROS介导的MSC的治疗机制仍然很大程度上未知。在这里,我们审查与细胞周期和染色质重塑相关的关键因素,以加速或延迟MSC衰老过程。此外,将与MSC衰老过程一起讨论增强的ROS产生及其相关的病理生理途径。此外,本综述强调了在ALI / ARDS和COPD的发病机理中,过量的ROS介导的氧化应激可能如何干扰肺和剩余肺细胞的稳态。

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