From the Department of Epidemiology, School of Public Health (N.S.C., E.B.L., L.D.C., M.R.I.), University of Alabama at Birmingham.
Division of Clinical Immunology and Rheumatology (S.L.B., K.G.S., E.J.R., J.R.C., A.G., R.J.R., J.A.S.), University of Alabama at Birmingham.
Hypertension. 2020 Jan;75(1):246-256. doi: 10.1161/HYPERTENSIONAHA.119.13580. Epub 2019 Dec 2.
Previous studies do not widely support hyperuricemia as a risk factor for stroke and other cardiovascular diseases. We assessed the relationship between hyperuricemia and ischemic stroke (≈900 cases) using a large data set from the REGARDS study (Reasons for Geographic and Racial Differences in Stroke). We employed a case-cohort design (incident stroke cases and randomly selected cohort participants) and weighted Cox-proportional hazard models to estimate the association of serum urate level ≥6.8 mg/dL (ie, hyperuricemia) and 6.0 to <6.8 mg/dL versus <6.0 mg/dL (reference) with incident stroke. Analyses were stratified by race, gender, and age. Mediation of cardiovascular disease comorbidities on the serum urate-stroke association was tested. Hyperuricemia was associated with stroke (hazard ratio, 1.40 [95% CI, 1.10-1.78]) after adjustment for demographic variables and systolic and diastolic blood pressure. This association was substantially attenuated (hazard ratio, 1.17 [95% CI, 0.90-1.51]) by additional covariate adjustment. In particular, apparent treatment-resistant hypertension (systolic blood pressure ≥140 mm Hg or diastolic blood pressure ≥90 mm Hg on 3 antihypertensive medications or use of ≥4 antihypertensive medications) and the count of antihypertensive medication classes significantly reduced the effect of hyperuricemia on ischemic stroke. Specifically, apparent treatment-resistant hypertension and number of antihypertensive, respectively, mediate 45% and 43% of the association. There was no effect modification in the association between hyperuricemia and stroke by age, race, or gender. We conclude that hyperuricemia may be a risk factor for stroke. The substantial attenuation of this association by apparent treatment-resistant hypertension and number of antihypertensive suggests that severe hypertension may be a mediator.
先前的研究并未广泛支持高尿酸血症是中风和其他心血管疾病的危险因素。我们使用 REGARDS 研究(中风地理和种族差异原因)的大型数据集,评估了高尿酸血症与缺血性中风(约 900 例)之间的关系。我们采用病例-队列设计(中风事件病例和随机选择的队列参与者)和加权 Cox 比例风险模型来估计血清尿酸水平≥6.8mg/dL(即高尿酸血症)和 6.0-<6.8mg/dL 与<6.0mg/dL(参考)与中风事件的关联。分析按种族、性别和年龄分层。测试了心血管疾病合并症对血清尿酸-中风关联的中介作用。在调整人口统计学变量、收缩压和舒张压后,高尿酸血症与中风相关(风险比,1.40[95%CI,1.10-1.78])。通过进一步调整协变量,这种关联明显减弱(风险比,1.17[95%CI,0.90-1.51])。特别是,明显的抗高血压药物抵抗性高血压(3 种抗高血压药物治疗时收缩压≥140mmHg 或舒张压≥90mmHg 或使用≥4 种抗高血压药物)和抗高血压药物类别的数量显著降低了高尿酸血症对缺血性中风的影响。具体来说,明显的抗高血压药物抵抗性高血压和抗高血压药物的数量分别介导了高尿酸血症与中风之间关联的 45%和 43%。高尿酸血症与中风之间的关联在年龄、种族或性别方面没有效应修饰。我们得出结论,高尿酸血症可能是中风的一个危险因素。这种关联明显减弱是由于明显的抗高血压药物抵抗性高血压和抗高血压药物的数量,表明严重的高血压可能是一种中介。