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接受家庭肠外营养且静脉注射较高剂量维生素C的患者,其尿草酸排泄量会增加。

Urinary oxalate excretion increases in home parenteral nutrition patients on a higher intravenous ascorbic acid dose.

作者信息

Peña de la Vega Lourdes, Lieske John C, Milliner Dawn, Gonyea Janelle, Kelly Darlene G

机构信息

Mayo Clinic Hyperoxaluria Center and the Mayo Clinic College of Medicine and Division of Nephrology, Department of Internal Medicine, Rochester, Minnesota 55905, USA.

出版信息

JPEN J Parenter Enteral Nutr. 2004 Nov-Dec;28(6):435-8. doi: 10.1177/0148607104028006435.

Abstract

BACKGROUND

Vitamin C can be metabolized to oxalate. Case reports have suggested an association between IV vitamin C and urinary oxalate excretion. Recently, the US Food and Drug Administration required the dose of vitamin C in IV multivitamin preparations to be increased from 100 mg to 200 mg/d. We compared the urinary oxalate excretion level in stable home total parenteral nutrition (TPN) patients receiving both doses of vitamin C.

METHODS

Each participant provided a 24-hour urine sample for oxalate determination on the vitamin C dose (100 mg/d), and again after at least 1 month on the increased vitamin C dose (200 mg/d). A 2-day diet diary was completed covering the day before and the day of the urine collection and was analyzed for oxalate and vitamin C content. Comparisons were made using Student paired t test and Wilcoxon signed rank.

RESULTS

Thirteen patients (7 males/6 females) aged 63.1 +/- 12.2 years who had no history of nephrolithiasis and had received TPN for 55.9 +/- 78.8 months were enrolled. The most common indication for TPN was short bowel syndrome (38.5%). Eight patients had an intact colon. Urinary oxalate excretion increased on the 200-mg vitamin C dose, from 0.34 +/- 0.13 to 0.44 +/- 0.17 mmol/d (mean increase = 0.10 mmol/d; p = .04; 95% confidence interval 0.004 to 0.19 mmol/d). Oral intake of vitamin C and oxalate did not differ between the 2 collection periods.

CONCLUSIONS

In therapeutically used doses, IV vitamin C increases urinary oxalate excretion, potentially predisposing susceptible individuals to nephrolithiasis. This factor should be considered in patients receiving home TPN.

摘要

背景

维生素C可代谢为草酸盐。病例报告提示静脉注射维生素C与尿草酸盐排泄之间存在关联。最近,美国食品药品监督管理局要求静脉用多种维生素制剂中维生素C的剂量从100毫克/天增加至200毫克/天。我们比较了接受这两种剂量维生素C的稳定家庭肠外营养(TPN)患者的尿草酸盐排泄水平。

方法

每位参与者在维生素C剂量为100毫克/天时提供一份24小时尿液样本用于草酸盐测定,在维生素C剂量增加至200毫克/天至少1个月后再次提供样本。完成一份涵盖尿液收集前一天和当天的2天饮食日记,并分析其中草酸盐和维生素C的含量。采用配对t检验和Wilcoxon符号秩检验进行比较。

结果

纳入了13例患者(7例男性/6例女性),年龄63.1±12.2岁,无肾结石病史,接受TPN治疗55.9±78.8个月。TPN最常见的适应证是短肠综合征(38.5%)。8例患者结肠完整。维生素C剂量为200毫克/天时,尿草酸盐排泄增加,从0.34±0.13毫摩尔/天增至0.44±0.17毫摩尔/天(平均增加 = 0.10毫摩尔/天;p = 0.04;95%置信区间0.004至0.19毫摩尔/天)。两个收集期之间口服维生素C和草酸盐摄入量无差异。

结论

在治疗剂量下,静脉注射维生素C会增加尿草酸盐排泄,可能使易感个体易患肾结石。接受家庭TPN治疗的患者应考虑这一因素。

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