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采用质谱法和 ELISA 法检测血液透析患者血清 hepcidin-25 的个体内变异性。

Intra-individual variability of serum hepcidin-25 in haemodialysis patients using mass spectrometry and ELISA.

机构信息

Department of Nephrology, Radboud University Nijmegen Medical Center, Nijmegen, The Netherlands.

出版信息

Nephrol Dial Transplant. 2012 Oct;27(10):3923-9. doi: 10.1093/ndt/gfs164. Epub 2012 Jul 19.

Abstract

BACKGROUND

Measurement of serum hepcidin levels may provide a useful alternative to the current methods of determining iron status in chronic haemodialysis (HD) patients. However, the biological variability of this pivotal regulator of iron homeostasis is unclear, and the impact of inflammation, dialysis clearance and iron therapy on hepcidin variability has not been established.

METHODS

Two independent studies in chronic HD patients were conducted; serum hepcidin levels were measured at the start of dialysis sessions in 20 UK patients and in 43 Dutch patients by mass spectrometry (MS). Samples from UK patients were also analysed by a competitive enzyme-linked immunosorbent assay (cELISA). Coefficient of variance (CV(1)) was calculated and potential factors affecting CV(1) were also examined.

RESULTS

The median CV(1) (inter-quartile range) was 23% (17-28) for the UK MS, 26% (17-48) for the Dutch MS and 23% (17-39) for the UK cELISA. The CV(1) was similar in those patients receiving and those not receiving regular intravenous iron. The CV(1) was not associated with the degree of inflammation. Hepcidin levels were higher following an inter-dialytic period of 3 versus 2 days (P = 0.02).

CONCLUSIONS

These findings suggest considerable variability of serum hepcidin levels in HD patients. Inflammation and the use of iron did not impact on the degree of variability, and hepcidin levels were higher after an inter-dialytic period of 3 versus 2 days. These findings need to be taken into account in future studies assessing the utility of serum hepcidin as a guide to the use of iron or erythropoiesis-stimulating agents therapy.

摘要

背景

血清铁调素水平的测量可能为慢性血液透析(HD)患者铁状态的当前测定方法提供有用的替代方法。然而,这种铁稳态关键调节剂的生物学变异性尚不清楚,炎症、透析清除率和铁治疗对铁调素变异性的影响尚未确定。

方法

对 20 名英国和 43 名荷兰慢性 HD 患者进行了两项独立研究;通过质谱法(MS)在透析开始时测量了这 20 名英国患者和 43 名荷兰患者的血清铁调素水平。英国患者的样本还通过竞争性酶联免疫吸附测定(cELISA)进行了分析。计算了变异系数(CV(1)),并检查了潜在影响 CV(1)的因素。

结果

英国 MS 的中位数 CV(1)(四分位距)为 23%(17-28),荷兰 MS 为 26%(17-48),英国 cELISA 为 23%(17-39)。接受和未接受常规静脉铁治疗的患者的 CV(1)相似。CV(1)与炎症程度无关。与 2 天相比,铁调素水平在 3 天的透间期后更高(P=0.02)。

结论

这些发现表明 HD 患者的血清铁调素水平存在相当大的变异性。炎症和铁的使用并没有影响变异性的程度,并且在 3 天的透间期后铁调素水平更高。在评估血清铁调素作为铁或促红细胞生成素刺激剂治疗的指导的效用的未来研究中,需要考虑到这些发现。

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