血管性血血病因子、可溶性p选择素和高血压靶器官损伤:盎格鲁-斯堪的纳维亚心脏结局试验(ASCOT)的一项亚研究

C. C. Spencer, D. Gurney, A. Blann, D. Beevers, G. Y. Lip
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引用次数: 85

摘要

为了研究血小板可溶性标志物、内皮和流变功能与靶器官损伤的关系及其对心血管并发症高危中年高血压患者强化治疗的反应,我们研究了382例连续患者(308例男性;平均年龄63岁,SD 8),血压正常且无心血管疾病的对照组60例。患者分为靶器官损伤组(TOD);N =107)和无终末器官损伤者。测定血浆可溶性p选择素(sP-sel)(血小板活化标志物)和血管性血友病因子(vWF)(内皮损伤/功能障碍指标)的水平(均采用酶联免疫吸附法),以及流变学指标纤维蛋白原、血浆粘度、红细胞压积、血小板和白细胞计数。在53例患者中,在加强心血管风险管理6个月后,进一步测量了变量。TOD患者的vWF明显更高,分别为137 (SD 33)和125 (SD 33) IU/dL (P =0.002),吸烟者的比例更高,分别为31%和16% (P =0.002)。两组患者血浆黏度、纤维蛋白原、红细胞压积、白细胞计数、血小板计数、sP-sel均无统计学差异。在多变量分析中,vWF是TOD的显著独立预测因子。53例入组患者经过6个月的强化治疗后,收缩压、总胆固醇、红细胞压积、血浆粘度、sP-sel和vWF均显著降低(P <0.01),但纤维蛋白原无显著变化。综上所述,高血压患者TOD与内皮损伤/功能障碍有关。强化治疗可改善血液流变学、内皮和血小板功能。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Von Willebrand Factor, Soluble P-Selectin, and Target Organ Damage in Hypertension: A Substudy of the Anglo-Scandinavian Cardiac Outcomes Trial (ASCOT)
To investigate the relationship between soluble markers of platelet, endothelial and rheological function, and target organ damage and their response to intensified management in a population of middle-age hypertensive patients at high risk of cardiovascular complications, we studied 382 consecutive patients (308 men; mean age, 63 years, SD 8) along with 60 normotensive controls free of cardiovascular disease. Patients were divided into those with target organ damage (TOD; n=107) and those free of end-organ damage. Plasma levels of soluble P-selectin (sP-sel), a marker of platelet activation, and von Willebrand factor (vWF), an index of endothelial damage/dysfunction (both enzyme-linked immunosorbent assay), and the rheological indices fibrinogen, plasma viscosity, hematocrit, platelet, and white cell count were measured. In 53 patients, variables were further measured after 6 months of intensified cardiovascular risk management. Patients with TOD had significantly higher vWF, 137 (SD 33) versus 125 (SD 33) IU/dL (P =0.002,) and a greater proportion of smokers, 31% versus 16% (P =0.002). There were no statistically significant differences in plasma viscosity, fibrinogen, hematocrit, white blood cell count, platelet count, or sP-sel between the 2 subgroups. In multivariate analysis, vWF was a significant independent predictor for TOD. After 6 months of intensified management in 53 patients who entered the trial, there were significant reductions in systolic blood pressure, total cholesterol, hematocrit, plasma viscosity, sP-sel, and vWF (all P <0.01) but no significant change in fibrinogen. In conclusion, there is a relationship between TOD and endothelial damage/dysfunction in hypertension. Intensified management results in improvements in hemorheology, endothelial and platelet function.
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