纤维蛋白原水平和心血管风险概况的个体差异性。

R S Rosenson, C C Tangney, J M Hafner
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引用次数: 47

摘要

前瞻性人群研究已经证实,纤维蛋白原是缺血性心脏病和中风的独立预测因子。这些研究结论促使人们建议将纤维蛋白原测定纳入心血管风险概况。纤维蛋白原测量的常规可用性可能导致在确定单个纤维蛋白原水平作为个体受试者准确描述的有效性之前进行广泛筛选。本研究的目的是描述使用Clauss方法测定的纤维蛋白原测量变异性的方法学和个体内成分;建立单一纤维蛋白原测量对风险分层和复验可重复性的有用性;并确定个体纤维蛋白原变异对样本量估计的影响。纤维蛋白原水平通过Clauss方法的改进来测量。招募了三组看起来健康、不吸烟的志愿者。在39名受试者中测定了纤维蛋白原变异的单日个体内成分。在为期5天的纤维蛋白原变异的个体内成分中,招募了32名受试者,在为期6周的个体内研究中,纳入了28名受试者。纤维蛋白原变异的方法学成分的变异系数为5.8%,这是通过批分析确定的,但在一天内重复测量的个体内变异系数为10.7%。5天的个体变异系数为14.2%,6周的个体变异系数为17.8%。根据6周的数据,平均需要4次纤维蛋白原测量才能将误分类误差降低到10%以下。样本量估计是基于预先确定的统计能力水平和6周的个体内和个体间变异性估计。(摘要删节250字)
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Intraindividual variability of fibrinogen levels and cardiovascular risk profile.

Prospective population studies have established that fibrinogen is an independent predictor for ischemic heart disease and stroke. These study conclusions have prompted recommendations that fibrinogen determinations be included in the cardiovascular risk profile. The routine availability of fibrinogen measurements may result in widespread screening prior to establishing the validity of a single fibrinogen level as an accurate descriptor for individual subjects. The objectives of this study were to describe the methodological and intraindividual components of variability in fibrinogen measurements determined by using the Clauss method; to establish the usefulness of a single fibrinogen measurement on risk stratification and retest reproducibility; and to determine the influence of intraindividual fibrinogen variability on sample size estimates. Fibrinogen levels were measured by a modification of the Clauss method. Three cohorts of apparently healthy, nonsmoking volunteers were recruited. The single-day intra-individual component of fibrinogen variability was determined in 39 subjects. For the 5-day intraindividual component of fibrinogen variability, 32 subjects were recruited, and in the 6-week intraindividual study, 28 subjects were included. The coefficient of variation for the methodological component of fibrinogen variability was 5.8% as determined from batch analyses, but the intraindividual coefficient of variation for replicate measures on a single day was 10.7%. The 5-day intraindividual coefficient of variation was 14.2%, and for the 6-week period it was 17.8%. Based on the 6-week data, an average of four fibrinogen measures is required to reduce misclassification error to less than 10%. Sample size estimates were made based on predetermined levels of statistical power and the 6-week intraindividual and interindividual variability estimates.(ABSTRACT TRUNCATED AT 250 WORDS)

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