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在稳定的血液透析患者中,骨特异性碱性磷酸酶浓度比甲状旁腺激素浓度变化小。

Bone-specific alkaline phosphatase concentrations are less variable than those of parathyroid hormone in stable hemodialysis patients.

机构信息

Clinical Biochemistry, East Kent Hospitals University NHS Foundation Trust, Kent and Canterbury Hospital, Canterbury, UK.

出版信息

Kidney Int. 2012 Jul;82(1):100-5. doi: 10.1038/ki.2012.77. Epub 2012 Mar 28.

Abstract

Abnormalities of bone mineral metabolism and vascular calcification are prevalent in patients with kidney failure. Clinical management is based on biochemical targets, in particular parathyroid hormone (PTH) concentrations, but this has many limitations including high biological variation. A possible alternative is bone-specific alkaline phosphatase (ALP); therefore, we evaluated the biological variation of this marker in patients undergoing hemodialysis. Bone ALP was measured in non-fasting serum samples taken twice a week over a 6-week period in 22 stable hemodialysis patients and 12 healthy volunteers. The within-individual coefficients of variance were calculated and used to derive the critical difference required to be certain that an observed change was significant. The coefficient of variance for bone ALP was significantly higher in hemodialysis patients compared to healthy individuals. Seven samples were required to estimate the homeostatic set point of bone ALP, within 10%, in a hemodialysis patient. The concentration of serial bone ALP measurements would need to change by 36% between any two measurements before it can be considered a significant change. Since the biological variation of bone ALP is less than half that reported for PTH, our study provides further support for the use of bone ALP as an alternative marker of bone mineral metabolism in the setting of chronic kidney disease-mineral and bone disorder.

摘要

骨矿物质代谢和血管钙化异常在肾衰竭患者中很常见。临床管理基于生化指标,特别是甲状旁腺激素(PTH)浓度,但这存在许多局限性,包括高生物学变异性。骨特异性碱性磷酸酶(ALP)可能是一种替代方法;因此,我们评估了接受血液透析的患者中该标志物的生物学变异性。在 22 名稳定血液透析患者和 12 名健康志愿者中,在 6 周的时间内,每周两次采集空腹血清样本测量骨 ALP。计算个体内变异系数,并用于得出确定观察到的变化是否显著所需的临界差异。与健康个体相比,骨 ALP 的血液透析患者的变异系数明显更高。在血液透析患者中,需要 7 个样本才能估计骨 ALP 的体内平衡点,在 10%以内。在两次测量之间,骨 ALP 的连续测量浓度需要变化 36%,才能被认为是显著变化。由于骨 ALP 的生物学变异性小于 PTH 报道的一半,因此我们的研究为在慢性肾脏病-矿物质和骨异常中使用骨 ALP 作为骨矿物质代谢的替代标志物提供了进一步的支持。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7ac3/3376309/ec6e9b41382a/ki201277f1.jpg

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