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非糖尿病患者血清尿酸水平升高标志着炎症状态和高密度脂蛋白功能障碍,并独立预测冠心病。

Elevated serum uric acid in nondiabetic people mark pro-inflammatory state and HDL dysfunction and independently predicts coronary disease.

机构信息

Turkish Society of Cardiology and Department of Cardiology, Cerrahpaşa Medical Faculty, Istanbul University, Istanbul, Turkey,

出版信息

Clin Rheumatol. 2013 Dec;32(12):1767-75. doi: 10.1007/s10067-013-2339-7. Epub 2013 Aug 11.

Abstract

We explored the association of serum uric acid (UA) concentrations with pro-inflammatory state and high-density lipoprotein (HDL) dysfunction. UA tertiles in tracked 1,508 nondiabetic participants were analyzed cross-sectionally for associations with inflammation biomarkers and protective proteins over a mean follow-up of 4.9 years for incident coronary heart disease (CHD) using Cox proportional hazards regression. In the absence of metabolic syndrome (MetS), UA tertiles significantly distinguished, in each sex, increasing categories of three MetS components (inflammation/oxidation markers, apolipoprotein (apo)B) and (inversely) current smoking (but not protective proteins such as HDL, apoA-I, and adiponectin). Distinctions attenuated in the presence of MetS. Linear regression model revealed fasting triglycerides (1.86 mg/dl variance), male sex, and gamma-glutamyl transferase and age as covariates of UA levels in women. In Cox analysis, incident CHD (n = 137) was predicted by mid and upper UA tertile in men alone at significant hazard ratios of 2.7, additively to conventional risk factors. Elevated serum UA levels, linked to triglycerides, mark in nondiabetic people pro-inflammatory state, and, notably, HDL dysfunction. CHD risk is independently predicted by elevated UA levels in nondiabetic men and is modulated by MetS and gender.

摘要

我们探讨了血清尿酸(UA)浓度与促炎状态和高密度脂蛋白(HDL)功能障碍的关系。在追踪的 1508 名非糖尿病参与者中,分析了第 1 至 3 尿酸三分位数与炎症生物标志物和保护性蛋白之间的关联,这些参与者在平均 4.9 年的时间内发生冠心病(CHD)的随访中使用 Cox 比例风险回归。在没有代谢综合征(MetS)的情况下,UA 三分位数在每个性别中均显著区分,随着三种 MetS 成分(炎症/氧化标志物、载脂蛋白(apo)B)和(相反)当前吸烟(但不是保护性蛋白,如 HDL、apoA-I 和脂联素)的增加类别而有所区分。在存在 MetS 的情况下,这种区别减弱了。线性回归模型显示空腹甘油三酯(1.86mg/dl 方差)、男性性别以及γ-谷氨酰转移酶和年龄是女性 UA 水平的协变量。在 Cox 分析中,仅在男性中,UA 中值和高值三分位数预测了 CHD 事件(n=137),其显著危险比为 2.7,与传统危险因素相加。非糖尿病患者中升高的血清 UA 水平与甘油三酯相关,标志着促炎状态,特别是 HDL 功能障碍。CHD 风险可通过非糖尿病男性中升高的 UA 水平独立预测,并且受到 MetS 和性别调节。

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