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血清磷酸盐是终末期肾病中校正血清钙的重要决定因素。

Serum phosphate is an important determinant of corrected serum calcium in end-stage kidney disease.

作者信息

Ferrari Paolo, Singer Richard, Agarwal Aanchal, Hurn Anne, Townsend Mary A, Chubb Paul

机构信息

Department of Nephrology, Fremantle Hospital, Perth, WA, Australia.

出版信息

Nephrology (Carlton). 2009 Jun;14(4):383-8. doi: 10.1111/j.1440-1797.2009.01121.x.

DOI:10.1111/j.1440-1797.2009.01121.x
PMID:19563379
Abstract

BACKGROUND

Approximately 12% of bound blood calcium is linked to various anions including phosphate. In patients with end-stage kidney disease (ESKD), serum phosphate is highly variable. We propose that establishing a formula to calculate albumin- and phosphate-corrected total calcium would be more appropriate to estimate free calcium in ESKD patients.

METHODS

In 82 haemodialysis patients, serum ionized calcium (Ca(ion)) and pH were measured by blood gas analyser with ion-selective electrodes at the point-of-care, while bicarbonate, phosphate, albumin, magnesium and total calcium (Ca(tot)) were measured at the central laboratory. Linear regression analysis of measured variables was used to best fit adjusted calcium versus Ca(ion).

RESULTS

The most parsimonious multiple linear regression model (r(2) = 0.81) of variables associated with Ca(ion) included Ca(tot) (coeff 0.820, P < 0.0001), albumin (coeff -0.016, P < 0.0001) and phosphate (coeff -0.063, P < 0.002). Modelling of available variables yielded the following equation to adjust calcium for albumin and phosphate: Ca(albPh) = Ca(tot) + (0.015 x (40 - [albumin]) + 0.07 x (1.5 - [phosphate])). At an ambient albumin of 40 g/L, Ca(albPh) would be 0.07 mmol/L lower than Ca(tot) for every mmol/L of phosphate. In vitro data using three different albumin levels and increasing phosphate concentrations demonstrated this relationship, with the slope of the phosphate effect being stronger at lower albumin concentrations.

CONCLUSION

Because guidelines recommendations indicate that corrected serum calcium should be maintained within the normal range in ESKD patients, inclusion of phosphate to correct Ca(tot) in these patients may have clinical implications on the choice of phosphate binders and the prescription of vitamin D or calcimimetic agents.

摘要

背景

约12%的结合血钙与包括磷酸盐在内的各种阴离子结合。在终末期肾病(ESKD)患者中,血清磷酸盐高度可变。我们提出,建立一个计算白蛋白和磷酸盐校正后总钙的公式,对于估计ESKD患者的游离钙更为合适。

方法

在82例血液透析患者中,使用离子选择性电极的血气分析仪在床旁测量血清离子钙(Ca(ion))和pH值,而碳酸氢盐、磷酸盐、白蛋白、镁和总钙(Ca(tot))在中心实验室测量。对测量变量进行线性回归分析,以最佳拟合校正钙与Ca(ion)的关系。

结果

与Ca(ion)相关的变量的最简约多元线性回归模型(r(2)=0.81)包括Ca(tot)(系数0.820,P<0.0001)、白蛋白(系数-0.016,P<0.0001)和磷酸盐(系数-0.063,P<0.002)。对可用变量进行建模得出以下用于校正白蛋白和磷酸盐的钙的公式:Ca(albPh)=Ca(tot)+(0.015×(40-[白蛋白])+0.07×(1.5-[磷酸盐]))。在白蛋白水平为40 g/L时,每毫摩尔/升的磷酸盐,Ca(albPh)比Ca(tot)低0.07毫摩尔/升。使用三种不同白蛋白水平和增加的磷酸盐浓度的体外数据证明了这种关系,在较低白蛋白浓度下磷酸盐效应的斜率更强。

结论

由于指南建议ESKD患者校正后的血清钙应维持在正常范围内,在这些患者中纳入磷酸盐以校正Ca(tot)可能对磷酸盐结合剂的选择以及维生素D或拟钙剂的处方具有临床意义。

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