Zinc Supplementation Trial in Pediatric Chronic Kidney Disease: Effects on Circulating FGF-23 and Klotho.

IF 1.6 Q3 UROLOGY & NEPHROLOGY Canadian Journal of Kidney Health and Disease Pub Date : 2024-03-13 eCollection Date: 2024-01-01 DOI:10.1177/20543581241234723
V Belostotsky, S A Atkinson, G Filler
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Abstract

Background: Zinc status, its role in bone metabolism and efficacy of deficiency correction has not been well studied in children with chronic kidney disease (CKD).

Objectives: The primary objective was to investigate whether 3 months of oral zinc supplementation corrects zinc deficiency in children with CKD who have native or transplanted kidneys. The secondary objective was to compare circulating intact FGF-23 (iFGF-23), c-terminal FGF-23 (cFGF-23), and Klotho between zinc-sufficient and zinc-deficient children with CKD and to assess the relationship between circulating zinc, iFGF-23, cFGF-23, Klotho, bone biomarkers, copper, and phosphate excretion pre-supplementation and post-supplementation of zinc.

Methods: Forty-one children (25 male and 16 female, age 12.94 ± 4.13 years) with CKD in native or transplanted kidneys were recruited through 2 pediatric nephrology divisions in Ontario, Canada. Of those, 14 patients (9 native CKD, 5 transplant CKD) with identified zinc deficiency (64% enrollment rate) received zinc citrate supplement for 3 months: 10 mg orally once (4-8 years) or twice (9-18 years) daily.

Results: Zinc deficiency (plasma concentration < 11.5 µmol/L) was found in 22 patients (53.7%). A linear regression model suggested that zinc concentration reduced by 0.026 µmol/L (P = .04) for every 1-unit of estimated glomerular filtration rate (eGFR) drop. Zinc deficiency status was associated with higher serum iFGF-23; however, this was predominantly determined by the falling GFR. Zinc deficient and sufficient children had similar circulating c-FGF-23 and alpha-Klotho. Normalization of plasma zinc concentration was achieved in 8 (5 native CKD and 3 transplant CKD) out of 14 treated patients rising from 10.04 ± 1.42 to 12.29 ± 3.77 μmol/L (P = .0038). There were no significant changes in other biochemical measures in all treated patients. A statistically significant (P = .0078) rise in c-FGF-23 was observed only in a subgroup of 11 children treated with zinc but not receiving calcitriol.

Conclusions: Zinc status is related to kidney function and possibly connected to bone metabolism in patients with CKD. However, it plays a minor role in fine-tuning various metabolic processes. In this exploratory non-randomized study, 3 months supplementation with zinc corrected deficiency in just over half of patients and only modestly affected bone metabolism in asymptomatic CKD patients.

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小儿慢性肾脏病补锌试验:对循环 FGF-23 和 Klotho 的影响
背景:对慢性肾脏病(CKD)儿童的锌状况、锌在骨代谢中的作用以及缺锌纠正的效果尚未进行深入研究:对于慢性肾脏病(CKD)患儿的锌状况、锌在骨代谢中的作用以及锌缺乏症的纠正效果尚未进行深入研究:主要目的是研究口服锌补充剂 3 个月是否能纠正原生肾脏或移植肾脏的 CKD 儿童的锌缺乏症。次要目的是比较锌充足和锌缺乏的 CKD 儿童血液中完整 FGF-23 (iFGF-23)、c-末端 FGF-23 (cFGF-23) 和 Klotho 的含量,并评估补锌前和补锌后血液中的锌、iFGF-23、cFGF-23、Klotho、骨生物标志物、铜和磷酸盐排泄量之间的关系:通过加拿大安大略省的两个儿科肾病科招募了 41 名患有原生肾脏或移植肾脏慢性肾功能衰竭的儿童(男 25 名,女 16 名,年龄为 12.94 ± 4.13 岁)。其中,14 名患者(9 名原发性 CKD,5 名移植性 CKD)被确认缺锌(入选率为 64%),接受了为期 3 个月的柠檬酸锌补充剂治疗:每天口服一次(4-8 岁)或两次(9-18 岁),每次 10 毫克:结果:22 名患者(53.7%)发现缺锌(血浆浓度小于 11.5 µmol/L)。线性回归模型表明,估计肾小球滤过率(eGFR)每下降 1 个单位,锌浓度就会降低 0.026 µmol/L(P = .04)。缺锌状态与血清 iFGF-23 的升高有关,但这主要取决于肾小球滤过率的下降。缺锌和足锌儿童的循环 c-FGF-23 和 alpha-Klotho 含量相似。在 14 名接受治疗的患者中,8 名(5 名原发性 CKD 和 3 名移植性 CKD)患者的血浆锌浓度从 10.04 ± 1.42 μmol/L 升至 12.29 ± 3.77 μmol/L(P = .0038),达到正常水平。所有接受治疗的患者的其他生化指标均无明显变化。只有在接受锌治疗但未服用降钙素三醇的11名儿童中,观察到c-FGF-23的上升具有统计学意义(P = .0078):结论:锌状况与肾功能有关,并可能与慢性肾脏病患者的骨代谢有关。结论:锌状况与肾功能有关,并可能与慢性肾脏病患者的骨代谢有关,但它在微调各种代谢过程中的作用较小。在这项探索性的非随机研究中,补锌 3 个月可纠正一半以上患者的锌缺乏症,对无症状的慢性肾功能衰竭患者的骨代谢影响不大。
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来源期刊
CiteScore
3.00
自引率
5.90%
发文量
84
审稿时长
12 weeks
期刊介绍: Canadian Journal of Kidney Health and Disease, the official journal of the Canadian Society of Nephrology, is an open access, peer-reviewed online journal that encourages high quality submissions focused on clinical, translational and health services delivery research in the field of chronic kidney disease, dialysis, kidney transplantation and organ donation. Our mandate is to promote and advocate for kidney health as it impacts national and international communities. Basic science, translational studies and clinical studies will be peer reviewed and processed by an Editorial Board comprised of geographically diverse Canadian and international nephrologists, internists and allied health professionals; this Editorial Board is mandated to ensure highest quality publications.
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