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The Oxidative Stress-Induced miR-200c Is Upregulated in Psoriasis and Correlates with Disease Severity and Determinants of Cardiovascular Risk

机译:氧化应激诱导的miR-200c在牛皮癣中上调,与心血管风险的疾病严重程度和决定因素相关联

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Psoriasis is a chronic inflammatory skin disease associated with reactive oxygen species (ROS) increase and a higher risk of cardiovascular (CV) events. We previously showed that the miR-200 family (miR-200s) is induced by ROS, miR-200c being the most upregulated member responsible for apoptosis, senescence, ROS increase, and nitric oxide decrease, finally causing endothelial dysfunction. Moreover, circulating miR-200c increases in familial hypercholesterolemic children and in plaques and plasma of atherosclerotic patients, two pathologies associated with increased ROS. Given miR-200s’ role in endothelial dysfunction, ROS, and inflammation, we hypothesized that miR-200s were modulated in lesional skin (LS) and plasma of psoriatic patients (Pso) and that their levels correlated with some CV risk determinants at a subclinical level. All Pso had severe psoriasis, i.e., Psoriasis Area and Severity Index PASI10, and one of the following: at least two systemic psoriasis treatments, age?at?onset40?years, and disease duration10?years. RNA was extracted from plasma (Pso, N=29; Ctrl, N=29) and from nonlesional skin (NLS) and LS of 6 Pso and 6 healthy subject skin (HS) biopsies. miR-200 levels were assayed by quantitative RT-PCR. We found that all miR-200s were increased in LS vs. NLS and miR-200c was the most expressed and upregulated in LS vs. HS. In addition, circulating miR-200c and miR-200a were upregulated in Pso vs. Ctrl. Further, miR-200c positively correlated with PASI, disease duration, left ventricular (LV) mass, LV relative wall thickness (RWT), and E/e′, a marker of diastolic dysfunction. Multiple regression analysis indicates a direct association between miR-200c and both RWT and LV mass. Circulating miR-200a correlated positively only with LV mass and arterial pressure augmentation index, a measure of stiffness, although the correlations were nearly significant (P=0.06). In conclusion, miR-200c is upregulated in LS and plasma of Pso, suggesting its role in ROS increase and inflammation associated with CV risk in psoriasis.
机译:牛皮癣是一种与反应性氧(ROS)相关的慢性炎症皮肤病,增加心血管(CV)事件的风险较高。我们以前表明,MIR-200家族(MIR-200S)由ROS诱导,MIR-200c是最具上调的成员,负责细胞凋亡,衰老,ROS增加和一氧化氮降低,最终导致内皮功能障碍。此外,循环miR-​​200c在家族性高胆固醇血症儿童中和动脉粥样硬化患者的斑块和血浆增加,两种病理学与ROS增加相关。在内皮功能障碍,ROS和炎症中,我们假设miR-200s在银屑病患者(PSO)的损伤皮肤(LS)和血浆中作用,并且它们的水平与亚临床的一些CV风险决定簇相关等级。所有PSO都有严重的牛皮癣,即牛皮癣面积和严重程度指数PASI> 10,以及以下之一:至少两个全身性牛皮癣治疗,年龄?AT?发病<40?年,疾病持续时间> 10?年。从血浆(PSO,N = 29; CTRL,N = 29)中提取RNA,从非缘皮肤(NLS)和6个PSO和6个健康受试者皮肤(HS)活组织检查。通过定量RT-PCR测定miR-200水平。我们发现,LS与NLS和MIR-200C中的所有miR-200s都是最表达和上调的。此外,在PSO与CTRL中循环miR-​​200c和miR-200a。此外,miR-200c与碱,疾病持续时间,左心室(LV)质量,LV相对壁厚(RWT)和E / E'正相关,舒张功能障碍的标志物。多元回归分析表明miR-200c和rwt和lv质量之间的直接关联。循环miR-​​200a仅通过LV质量和动脉压延指数,刚度的衡量标准相关,尽管相关性几乎显着(p = 0.06)。总之,MIR-200C在PSO的LS和血浆中上调,表明其在ROS的作用和牛皮癣中与CV风险相关的炎症。

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