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较高的尿皮质醇水平与心血管风险增加相关。

Higher urinary cortisol levels associate with increased cardiovascular risk.

作者信息

Haas Andrea V, Hopkins Paul N, Brown Nancy J, Pojoga Luminita H, Williams Jonathan S, Adler Gail K, Williams Gordon H

机构信息

Division of Endocrinology, Diabetes and Hypertension, Department of Medicine, Brigham and Women's Hospital, Harvard Medical School, Boston, Massachusetts, USA.

Cardiovascular Genetics, Department of Internal Medicine, University of Utah School of Medicine, Salt Lake City, Utah, USA.

出版信息

Endocr Connect. 2019 Jun 1;8(6):634-640. doi: 10.1530/EC-19-0182.

Abstract

There are conflicting data on whether variations of physiologic cortisol levels associated with cardiovascular risk. We hypothesize that prior discordant findings are related to problems associated with varying sample size, techniques for assessing cardiovascular risk and failure to adequately account for environmental factors. To address these issues, we utilized a large sample size, selected the Framingham risk score to compute cardiovascular risk and performed the study in a highly controlled setting. We had two main objectives: determine whether higher, yet physiologic, cortisol levels associated with increased cardiovascular risk and determine whether caveolin-1 (rs926198) risk allele carriers associated with increased cardiovascular risk. This was a cross-sectional study of 574 non-diabetic individuals who completed a common protocol. Data collection included fasting blood samples, blood pressure measurements and a 24-h urine-free cortisol collection. Five hundred seventeen of these participants also completed caveolin-1 genotyping. Subjects were classified as belonging to either the low-mode or high-mode urine-free cortisol groups, based on the bimodal distribution of urine-free cortisol. In multivariate analysis, Framingham risk score was statistically higher in the high-mode cortisol group (10.22 (mean) ± 0.43 (s.e.m.)) compared to the low-mode cortisol group (7.73 ± 0.34), P < 0.001. Framingham risk score was also statistically higher in the caveolin-1 risk allele carriers (8.91 ± 0.37) compared to caveolin-1 non-risk allele carriers (7.59 ± 0.48), P = 0.034. Overall, the estimated effect on Framingham risk score of carrying the caveolin-1 risk allele was 1.33 ± 0.61, P = 0.029. Both urinary cortisol and caveolin-1 risk allele status are independent predictors of Framingham risk score.

摘要

关于生理皮质醇水平的变化是否与心血管风险相关,存在相互矛盾的数据。我们推测,之前不一致的研究结果与样本量不同、评估心血管风险的技术以及未能充分考虑环境因素等问题有关。为了解决这些问题,我们采用了大样本量,选择弗雷明汉风险评分来计算心血管风险,并在高度可控的环境中进行了这项研究。我们有两个主要目标:确定较高但仍处于生理水平的皮质醇水平是否与心血管风险增加相关,以及确定小窝蛋白-1(rs926198)风险等位基因携带者是否与心血管风险增加相关。这是一项对574名完成共同方案的非糖尿病个体进行的横断面研究。数据收集包括空腹血样、血压测量以及24小时无尿皮质醇收集。其中517名参与者还完成了小窝蛋白-1基因分型。根据无尿皮质醇的双峰分布,受试者被分类为属于低模式或高模式无尿皮质醇组。在多变量分析中,与低模式皮质醇组(7.73±0.34)相比,高模式皮质醇组(平均值为10.22±0.43(标准误))的弗雷明汉风险评分在统计学上更高,P<0.001。与小窝蛋白-1非风险等位基因携带者(7.59±0.48)相比,小窝蛋白-1风险等位基因携带者(8.91±0.37)的弗雷明汉风险评分在统计学上也更高,P = 0.034。总体而言,携带小窝蛋白-1风险等位基因对弗雷明汉风险评分的估计影响为1.33±0.61,P = 0.029。尿皮质醇和小窝蛋白-1风险等位基因状态都是弗雷明汉风险评分的独立预测因素。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/932a/6528405/cfb34f283cab/EC-19-0182fig1.jpg

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