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蛋白尿相关的肾脏镁丢失导致低镁血症:慢性肾脏病常见的电解质异常。

Proteinuria-associated renal magnesium wasting leads to hypomagnesemia: a common electrolyte abnormality in chronic kidney disease.

机构信息

Department of Nephrology, Osaka University Graduate School of Medicine, Osaka, Japan.

Department of Inter-Organ Communication Research in Kidney Disease, Osaka University Graduate School of Medicine, Osaka, Japan.

出版信息

Nephrol Dial Transplant. 2019 Jul 1;34(7):1154-1162. doi: 10.1093/ndt/gfy119.

Abstract

BACKGROUND

Hypomagnesemia (Hypo-Mg) predicts mortality and chronic kidney disease (CKD) progression. However, in CKD, its prevalence, kidney-intrinsic risk factors, and the effectiveness of oral magnesium (Mg) therapy on serum Mg levels is uncertain.

METHODS

In a cross-sectional study enrolling pre-dialysis outpatients with CKD, the prevalence of electrolyte abnormalities (Mg, sodium, potassium, calcium and phosphorus) was compared. In an open-label randomized controlled trial (RCT), we randomly assigned CKD patients to either the magnesium oxide (MgO) or control arm. The outcome was serum Mg levels at 1 year.

RESULTS

In 5126 patients, Hypo-Mg was the most common electrolyte abnormality (14.7%) with similar prevalence across stages of CKD. Positive proteinuria was a risk factor of Hypo-Mg (odds ratio 2.2; 95% confidence interval 1.2-4.0). However, stratifying the analyses by diabetes mellitus (DM), it was not significant in DM (Pinteraction = 0.04). We enrolled 114 patients in the RCT. Baseline analyses showed that higher proteinuria was associated with higher fractional excretion of Mg. This relationship between proteinuria and renal Mg wasting was mediated by urinary tubular markers in mediation analyses. In the MgO arm, higher proteinuria or tubular markers predicted a significantly lower 1-year increase in serum Mg. In patients with a urinary protein-to-creatinine ratio (uPCR) <0.3 g/gCre, serum Mg at 1 year was 2.4 and 2.0 mg/dL in the MgO and control arms, respectively (P < 0.001), with no significant between-group difference in patients whose uPCR was ≥0.3 g/gCre (Pinteraction=0.001).

CONCLUSIONS

Proteinuria leads to renal Mg wasting through tubular injuries, which explains the high prevalence of Hypo-Mg in CKD.

摘要

背景

低镁血症(Hypo-Mg)可预测死亡率和慢性肾脏病(CKD)进展。然而,在 CKD 中,其患病率、肾脏内在危险因素以及口服镁(Mg)治疗对血清 Mg 水平的有效性尚不确定。

方法

在一项纳入透析前 CKD 门诊患者的横断面研究中,比较了电解质异常(Mg、钠、钾、钙和磷)的患病率。在一项开放标签随机对照试验(RCT)中,我们将 CKD 患者随机分配至氧化镁(MgO)或对照组。主要结局为 1 年时的血清 Mg 水平。

结果

在 5126 例患者中,Hypo-Mg 是最常见的电解质异常(14.7%),在 CKD 各阶段的患病率相似。蛋白尿阳性是 Hypo-Mg 的危险因素(优势比 2.2;95%置信区间 1.2-4.0)。然而,按糖尿病(DM)分层分析,在 DM 中无统计学意义(P 交互=0.04)。我们在 RCT 中纳入了 114 例患者。基线分析显示,更高的蛋白尿与更高的 Mg 分数排泄有关。在中介分析中,蛋白尿和肾镁丢失之间的这种关系是由尿管状标志物介导的。在 MgO 组中,更高的蛋白尿或管状标志物预测血清 Mg 在 1 年内的增加显著降低。在尿蛋白与肌酐比值(uPCR)<0.3 g/gCre 的患者中,MgO 组和对照组 1 年后的血清 Mg 分别为 2.4 和 2.0 mg/dL(P<0.001),而 uPCR≥0.3 g/gCre 的患者两组之间无显著差异(P 交互=0.001)。

结论

蛋白尿通过管状损伤导致肾镁丢失,这解释了 CKD 中 Hypo-Mg 患病率高的原因。

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