Levey A S, Greene T, Schluchter M D, Cleary P A, Teschan P E, Lorenz R A, Molitch M E, Mitch W E, Siebert C, Hall P M
National Institute of Diabetes and Digestive and Kidney Diseases, National Institutes of Health, Bethesda, MD.
J Am Soc Nephrol. 1993 Nov;4(5):1159-71. doi: 10.1681/ASN.V451159.
To assess the utility and precision of GFR measurements in multicenter trials, the test performance and variability of GFR were analyzed in 2,250 patients enrolled in 44 clinical centers participating in either the Modification of Diet in Renal Disease (MDRD) Study or the Diabetes Control and Complications Trial (DCCT). GRF was measured as the renal clearance of [125I]iothalamate after an sc injection without epinephrine. The studies used similar protocols for obtaining blood and urine, training clinical center staff, and processing specimens in central laboratories. The performance of GFR measurements, assessed from adherence to protocol and quality control analyses, was excellent. The variability among the four clearance periods (intratest coefficient of variation [CV]) was acceptable; the median intratest CV for GFR was 9.4% in the MDRD Study and 11.7% in the DCCT. The pattern of decline in serum counts was better approximated by an exponential rather than a linear relationship. The cause of the intratest variability in GFR measurements was explored by univariate and multivariate analysis. The intratest CV was highest at the extremes of GFR. Among patients with a high GFR (> 90 mL/min per 1.73 m2), most of whom were participants in the DCCT, the higher intratest GFR was due, in part, to a systematic decline in GFR during the test. Among patients with a very low GFR (< 13 mL/min per 1.73 m2), technical difficulties in urine collections contributed substantially to the higher intratest CV. Other patient characteristics, including age, gender, weight, serum glucose, renal diagnosis, and use of diuretics, were not strongly correlated with the intratest CV. The precision of GFR measurements was assessed from the variability from measurement to measurement (interest CV). Among MDRD Study subjects, in whom two measurements of GFR were performed over a 3-month interval, the median interest CV was relatively low (6.3%) and was only weakly related to the intratest CV. Thus, GFR measurements are reasonably precise, even if the intratest CV is high. Given the relatively high intratest CV that is characteristic of GFR measurements, the estimate of GFR in an individual is more precise if multiple clearance periods, rather than a single period, are included. Similarly, the estimate of mean GFR for a population is also more precise if multiple clearance periods are included. In conclusion, by the use of standardized methods, an acceptable precision of GFR results can be obtained in multicenter trials. The same methods can be applied in clinical practice.(ABSTRACT TRUNCATED AT 400 WORDS)
为评估肾小球滤过率(GFR)测量值在多中心试验中的效用和精确性,对参与肾脏病饮食改良(MDRD)研究或糖尿病控制与并发症试验(DCCT)的44个临床中心的2250例患者的GFR测试性能和变异性进行了分析。GFR通过皮下注射不含肾上腺素的[125I]碘肽酸盐后的肾脏清除率来测量。这些研究在获取血液和尿液、培训临床中心工作人员以及在中心实验室处理标本方面采用了相似的方案。从方案依从性和质量控制分析评估的GFR测量性能非常出色。四个清除期之间的变异性(测试内变异系数[CV])是可接受的;MDRD研究中GFR的测试内CV中位数为9.4%,DCCT中为11.7%。血清计数下降模式用指数关系而非线性关系能更好地拟合。通过单变量和多变量分析探讨了GFR测量中测试内变异性的原因。测试内CV在GFR的极端值时最高。在GFR高(>90 ml/min per 1.73 m2)的患者中,其中大多数是DCCT的参与者,测试内GFR较高部分是由于测试期间GFR的系统性下降。在GFR非常低(<13 ml/min per 1.73 m2)的患者中,尿液收集的技术困难对测试内较高的CV有很大影响。其他患者特征,包括年龄、性别、体重、血糖、肾脏诊断和利尿剂的使用,与测试内CV没有很强的相关性。GFR测量的精确性通过测量之间的变异性(感兴趣CV)来评估。在MDRD研究对象中,在3个月间隔内进行了两次GFR测量,感兴趣CV中位数相对较低(6.3%),且与测试内CV仅有微弱关联。因此,即使测试内CV较高,GFR测量仍相当精确。鉴于GFR测量具有相对较高的测试内CV,如果纳入多个清除期而非单个清除期,个体GFR的估计会更精确。同样,如果纳入多个清除期,人群平均GFR的估计也会更精确。总之,通过使用标准化方法,在多中心试验中可获得可接受的GFR结果精确性。相同方法可应用于临床实践。(摘要截断于400字)
