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首页> 外文期刊>American Journal of Kidney Diseases: The official journal of the National Kidney Foundation >Day-to-day variability in spot urine protein-creatinine ratio measurements
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Day-to-day variability in spot urine protein-creatinine ratio measurements

机译:尿液中尿蛋白-肌酐比值的每日变化

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Background: Accurate measurement of proteinuria is important in the diagnosis and management of chronic kidney disease (CKD). The reference standard test, 24-hour urinary protein excretion, is inconvenient and vulnerable to collection errors. Spot urine protein-creatinine ratio (PCR) is a convenient alternative and is in widespread use. However, day-to-day variability in PCR measurements has not been evaluated. Study Design: Prospective cohort study of day-to-day variability in spot urine PCR measurement. Setting & Participants: Clinically stable outpatients with CKD (n = 145) attending a university hospital CKD clinic in Australia between July 2007 and April 2010. Index Test: Spot urine PCR. Outcomes: Spot PCR variability was assessed and repeatability limits were determined using fractional polynomials. Measurements: Spot PCRs were measured from urine samples collected at 9:00 am on consecutive days and 24-hour urinary protein excretion was collected concurrently. Results: Paired results were analyzed from 145 patients: median age, 56 years; 59% men; and median 24-hour urinary protein excretion, 0.7 (range, 0.06-35.7) g/d. Day-to-day variability was substantial and increased in absolute terms, but decreased in relative terms with increasing baseline PCR. For patients with a low baseline PCR (20 mg/mmol [177 mg/g]), a change greater than ±160% (repeatability limits, 0-52 mg/mmol [0-460 mg/g]) is required to indicate a real change in proteinuria status with 95% certainty, whereas for those with a high baseline PCR (200 mg/mmol [1,768 mg/g]), a change of ±50% (decrease to <100 mg/mmol [<884 mg/g] or increase to >300 mg/mmol [>2,652 mg/g]) represents significant change. Limitations: These study results need to be replicated in other ethnic groups. Conclusions: Changes in PCR observed in patients with CKD, ranging from complete resolution to doubling of PCR values, could be due to inherent biological variation and may not indicate a change in disease status. This should be borne in mind when using PCR in the diagnosis and management of CKD.
机译:背景:蛋白尿的准确测量对慢性肾脏病(CKD)的诊断和治疗很重要。参考标准测试(24小时尿蛋白排泄)不方便且容易出现采集错误。尿蛋白-肌酐比值测定法(PCR)是一种方便的替代方法,已被广泛使用。但是,尚未评估PCR测量中的日常变异性。研究设计:前瞻性队列研究点尿PCR检测中日常变化。场所和参与者:2007年7月至2010年4月间在澳大利亚的大学医院CKD诊所就诊的临床稳定的CKD门诊患者(n = 145)。指标测试:尿液PCR检测。结果:评估了点PCR的变异性,并使用分数多项式确定了重复性极限。测量:连续9天从上午9:00收集的尿液样品中检测点PCR,并同时收集24小时尿蛋白排泄量。结果:对来自145例患者的配对结果进行了分析:中位年龄56岁;平均年龄56岁。 59%的男性;和24小时尿蛋白排泄量的中位数为0.7(范围为0.06-35.7)g / d。日常变异性很大,绝对值增加,但随着基线PCR的增加相对值降低。对于低基线PCR(20 mg / mmol [177 mg / g])的患者,要求变化大于±160%(可重复性极限,0-52 mg / mmol [0-460 mg / g])表明蛋白尿状态的真实变化具有95%的确定性,而基线PCR高(200 mg / mmol [1,768 mg / g])的人,其变化为±50%(降低至<100 mg / mmol [<884 mg / g]或增加至> 300 mg / mmol [> 2,652 mg / g])表示有显着变化。局限性:这些研究结果需要在其他种族中复制。结论:CKD患者观察到的PCR变化,从完全分离到PCR值翻倍,可能是由于固有的生物学差异,可能并不表示疾病状态的改变。使用PCR诊断和管理CKD时应牢记这一点。

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