血清硬化蛋白与复发性肾结石形成相关,独立于高钙尿症

NDT Plus Pub Date : 2023-11-01 DOI:10.1093/ckj/sfad256
Daniel Rodríguez, Ekaterina Gurevich, Soroush Mohammadi Jouabadi, Eva Maria Pastor Arroyo, Alexander Ritter, Sandrine Estoppey Younes, Carsten A Wagner, Pedro Henrique Imenez Silva, Harald Seeger, Nilufar Mohebbi
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As hypercalciuria is one of the most relevant risk factors for kidney stones, sclerostin might possess pathogenic relevance in nephrolithiasis. Methods We performed a prospective cross-sectional observational controlled study in 150 recurrent kidney stone formers (rKSF) to analyse the association of sclerostin with known stone risk factors and important modulators of calcium-phosphate metabolism. Serum sclerostin levels were determined at the first visit. As controls, we used 388 non-stone formers from a large Swiss epidemiological cohort. Results Sclerostin was mildly increased in rKSF in comparison to controls. This finding was more pronounced in women compared to men. Logistic regression indicated an association of serum sclerostin with rKSF status. In hypercalciuric individuals, sclerostin levels were not different from normocalciuric patients. In Spearman correlation analysis we found a positive correlation between sclerostin, age, and BMI and a negative correlation with eGFR. 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摘要

背景肾结石在工业化国家很常见,其终生风险为10 - 15%。高百分比的个体经历复发。含钙结石占肾结石的80%以上。饮食、环境因素、行为和基因变异都会导致肾结石的发生。骨细胞分泌21 kDa的糖蛋白硬化蛋白,抑制成骨细胞的骨形成。动物数据表明,硬化蛋白可能直接或间接调节钙通过肾脏的排泄。由于高钙尿症是肾结石最相关的危险因素之一,硬化蛋白可能在肾结石中具有致病相关性。方法:我们对150例复发性肾结石患者(rKSF)进行了一项前瞻性横断面观察对照研究,以分析硬化蛋白与已知的结石危险因素和重要的磷酸钙代谢调节剂的关系。第一次就诊时测定血清硬化蛋白水平。作为对照,我们从一个大型瑞士流行病学队列中选取388名非结石患者。结果与对照组相比,硬化素在rKSF中轻度升高。与男性相比,这一发现在女性身上更为明显。Logistic回归显示血清硬化蛋白与rKSF状态相关。在高钙血症个体中,硬化蛋白水平与正常钙血症患者没有差异。在Spearman相关分析中,我们发现硬化蛋白、年龄和BMI呈正相关,与eGFR呈负相关。与iPTH和完整fgf23的相关性较弱。相比之下,血清硬化蛋白水平与25-OH维生素D3、1,25-二羟基维生素D3、尿钙和磷酸盐或其他尿结石危险因素无关。结论:这是第一个研究rKSF患者血清硬化蛋白的前瞻性对照研究。在rKSF中,硬化蛋白水平升高与高钙尿无关,且与rKSF状态显著相关。似乎高钙尿症以外的机制可能参与其中,因此需要进一步的研究来阐明潜在的途径。
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Serum sclerostin is associated with recurrent kidney stone formation independent of hypercalciuria
ABSTRACT Background Kidney stones are frequent in industrialized countries with a lifetime risk of 10 to 15%. A high percentage of individuals experience recurrence. Calcium-containing stones account for more than 80% of kidney stones. Diet, environmental factors, behavior, and genetic variants contribute to the development of kidney stones. Osteocytes excrete the 21 kDa glycoprotein sclerostin, which inhibits bone formation by osteoblasts. Animal data suggests that sclerostin might directly or indirectly regulate calcium excretion via the kidney. As hypercalciuria is one of the most relevant risk factors for kidney stones, sclerostin might possess pathogenic relevance in nephrolithiasis. Methods We performed a prospective cross-sectional observational controlled study in 150 recurrent kidney stone formers (rKSF) to analyse the association of sclerostin with known stone risk factors and important modulators of calcium-phosphate metabolism. Serum sclerostin levels were determined at the first visit. As controls, we used 388 non-stone formers from a large Swiss epidemiological cohort. Results Sclerostin was mildly increased in rKSF in comparison to controls. This finding was more pronounced in women compared to men. Logistic regression indicated an association of serum sclerostin with rKSF status. In hypercalciuric individuals, sclerostin levels were not different from normocalciuric patients. In Spearman correlation analysis we found a positive correlation between sclerostin, age, and BMI and a negative correlation with eGFR. There was a weak correlation with iPTH and intact FGF 23. In contrast, serum sclerostin levels were not associated with 25-OH Vitamin D3, 1,25-dihydroxy-Vitamin D3, urinary calcium and phosphate or other urinary lithogenic risk factors. Conclusion This is the first prospective controlled study investigating serum sclerostin in rKSF. Sclerostin levels were increased in rKSF independent of hypercalciuria and significantly associated with the status as rKSF. It appears that mechanisms other than hypercalciuria may be involved and thus further studies are required to elucidate underlying pathways.
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