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首页> 外文期刊>Journal of Thrombosis and Thrombolysis >Microalbuminuria, von Willebrand factor and fibrinogen levels as markers of the severity in COPD exacerbation
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Microalbuminuria, von Willebrand factor and fibrinogen levels as markers of the severity in COPD exacerbation

机译:微量白蛋白尿,von Willebrand因子和纤维蛋白原水平是COPD恶化严重程度的标志

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摘要

In COPD, the systemic effects of the disease reflect the structural and/or biochemical alterations occurring in the structures or organs other than the lungs in relation to the characteristics of the primary disease. The disorders of endothelial structures due to COPD may lead vascular pathologies, such as ischemic heart disease, stroke, to occur more commonly in those with COPD. On consideration of the fact that the vascular endothelium is a major site in which the systemic effect of the inflammation occurs, should von Willebrand Factor, a clotting factor of endothelium origin, and the plasma level of fibrinogen vary with the severity of the disease in COPD, the variability of arterial blood gas values, and the stability or exacerbation of the disease? Considering the fact that microalbuminuria is an indirect manifestation of the renal endothelial permeability and/or renal perfusion; should there be an association between microalbuminuria and the severity of COPD? Therefore, in order to assess the effect of the systemic inflammation in COPD on the vascular endothelium, we compared the levels of the plasma vWF, fibrinogen, 24-h urine microalbuminuria of those with stable COPD (33 patients) and exacerbation of COPD (26 patients) with those of the controls (16 healthy subjects). The mean age was 63.42 ? 10.29, 68.00 ? 9.77 and 59.63 ? 14.10 years in SCOPD, COPDAE, and CG, respectively. The level of microalbuminuria was found to increase significantly in COPDAE group, compared to that of the controls (P = 0.004). When we investigated the relation between smoking burden and microalbuminuria, vWF, fibrinogen levels, the amount of consumption and positive relationship were found significant. (r = 0.336, P = 0.003 between smoking pack-years and vWF, r = 0.403, P = 0.001 between smoking pack-years and fibrinogen, and r = 0.262, P = 0.02 between smoking pack-years and microalbuminuria). The levels of vWF and fibrinogen are AECOPD > SCOPD > CG, with the highest being in AECOPD, and the difference among the groups was statistically significant. The relationship between the level of hypoxemia and microalbuminuria, fibrinogen and vWF was found to be significant (r = ?0.360, P = 0.005 between oxygen saturation and microalbuminuria, r = ?0.359, P = 0.005 between the level of PaO2 and fibrinogen, and r = ?0.336, P = 0.009 between PaO2 and vWF). In conclusion, the levels of plasma vWF, fibrinogen, and microalbuminuria may be helpful in grading the severity of COPD exacerbation. The related increase in these markers may represent a possible pathophysiological mechanism behind the increased vascular morbidity of patients with COPD and detecting indirectly the endothelial dysfunction as a manifestation of systemic outcomes due to COPD and in detecting earlier the cases in which the risk for developing the associated complications are higher. We suggest that further studies are necessary to investigate the impact of antithrombotic treatment on microalbuminuria, plasma vWF and fibrinogen as markers of endothelial dysfunction coexisting COPD exacerbation.
机译:在COPD中,疾病的全身作用反映了与原发疾病特征相关的,除肺外的结构或器官中发生的结构和/或生化改变。 COPD引起的内皮结构紊乱可能导致血管病变,例如缺血性心脏病,中风,在患有COPD的患者中更常见。考虑到血管内皮是炎症发生全身性作用的主要部位这一事实,是否应将血管源性凝血因子von Willebrand因子和血浆纤维蛋白原水平随COPD疾病的严重程度而变化,动脉血气值的可变性以及疾病的稳定性或恶化?考虑到微量白蛋白尿是肾内皮通透性和/或肾灌注的间接表现;微量白蛋白尿与COPD的严重程度之间是否存在关联?因此,为了评估COPD中全身性炎症对血管内皮的影响,我们比较了稳定COPD(33例)和COPD恶化的血浆血浆vWF,纤维蛋白原,24小时尿微量白蛋白水平(26患者)与对照组(16名健康受试者)的对照。平均年龄是63.42岁? 10.29、68.00? 9.77和59.63?分别在SCOPD,COPDAE和CG工作了14.10年。与对照组相比,发现COPDAE组的微量白蛋白尿水平显着增加(P = 0.004)。当我们调查吸烟负担与微量白蛋白尿,vWF,纤维蛋白原水平之间的关系时,发现摄入量与正相关性显着。 (r = 0.336,在吸烟者年与vWF之间,P = 0.003,r = 0.403,在吸烟者年与纤维蛋白原之间,P = 0.001,r = 0.262,在吸烟者-年与微量白蛋白尿之间,P = 0.02)。 vWF和纤维蛋白原的水平为AECOPD> SCOPD> CG,其中AECOPD最高,各组之间的差异具有统计学意义。低氧血症水平与微量白蛋白尿,纤维蛋白原和vWF之间存在显着相关性(氧饱和度与微量白蛋白尿之间r = 0.360,P = 0.005,PaO2水平之间r = 0.359,P = 0.005 和纤维蛋白原,且PaO2和vWF之间的r =α0.336,P = 0.009)。总之,血浆vWF,纤维蛋白原和微量白蛋白尿的水平可能有助于分级COPD恶化的严重程度。这些标志物的相关增加可能代表了COPD患者血管发病率增加背后的可能的病理生理机制,并间接检测出内皮功能障碍是由于COPD引起的系统性结局的表现,并且在更早发现发生相关疾病风险的情况下并发症较高。我们建议进一步的研究是必要的,以研究抗血栓形成治疗对微量白蛋白尿,血浆vWF和纤维蛋白原的影响,作为内皮功能障碍的标志物与COPD恶化并存。

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