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健康不吸烟人群尿样中尿镉排泄的变异性:在研究设计中的意义。

Variability of urinary cadmium excretion in spot urine samples, first morning voids, and 24 h urine in a healthy non-smoking population: implications for study design.

机构信息

Department of Occupational and Environmental Medicine, Sahlgrenska University Hospital and Academy, University of Gothenburg, Gothenburg, Sweden.

Department of Occupational and Environmental Medicine, Lund University Hospital, Lund, Sweden.

出版信息

J Expo Sci Environ Epidemiol. 2014 Mar-Apr;24(2):171-9. doi: 10.1038/jes.2013.58. Epub 2013 Sep 11.

Abstract

When selecting the least biased exposure surrogate, for example, the concentration of a biomarker in a urine sample, information on variability must be taken into consideration. We used mixed-effects models to estimate the variability and determinants of urinary cadmium (U-Cd) excretion using spot urine samples collected at six fixed times during 2 days about 1 week apart, from 24 healthy non-smokers. The urine samples were analysed for U-Cd, the concentrations were adjusted for dilution, and the excretion rates were calculated. Between-individual variability dominated the total variability for most measures of U-Cd excretion, especially for 24 h urine and first morning samples. The U-Cd excretion showed a circadian rhythm during the day, and time point of sampling was a significant factor in the mixed-effects models, thus a standardised sampling time, such as first morning urine samples, needs to be applied. Gender, urinary flow rate, age, and urinary protein excretions were also significant determinants for U-Cd excretion. The choice of biomarker for U-Cd excretion was found to be more important in individually-based studies of exposure-response relationships than in studies of comparing Cd levels of groups. When planning a study, this variability of U-Cd in spot samples must be acknowledged.

摘要

在选择最小偏差的暴露替代物(例如,尿液样本中的生物标志物浓度)时,必须考虑到变异性信息。我们使用混合效应模型,利用 24 名健康不吸烟者在相隔约 1 周的 2 天内的 6 个固定时间点收集的尿液样本,估算了尿液中镉(U-Cd)排泄的变异性及其决定因素。尿液样本用于分析 U-Cd,浓度经稀释调整后,计算排泄率。对于 U-Cd 排泄的大多数测量值,个体间变异性主导着总变异性,尤其是 24 小时尿液和晨尿。U-Cd 排泄在白天呈现出昼夜节律,采样时间点是混合效应模型中的一个重要因素,因此需要采用标准化的采样时间,如晨尿。性别、尿流量、年龄和尿蛋白排泄也是 U-Cd 排泄的重要决定因素。研究发现,在基于个体的暴露反应关系研究中,生物标志物的选择比在比较组间 Cd 水平的研究中更为重要。在计划研究时,必须承认这种点样尿液中 U-Cd 的变异性。

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