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Urinary oxalate excretion in urolithiasis and nephrocalcinosis.

机译:尿石症和肾钙化病中尿草酸盐的排泄。

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AIMS: To investigate urinary oxalate excretion in children with urolithiasis and/or nephrocalcinosis and to classify hyperoxaluria (HyOx). METHODS: A total of 106 patients were screened. In those in whom the oxalate: creatinine ratio was increased, 24 hour urinary oxalate excretion was measured. Liver biopsy and/or genomic analysis was performed if primary hyperoxaluria (PH) was suspected. Stool specimens were examined for Oxalobacter formigenes in HyOx not related to PH type 1 or 2 (PH1, PH2) and in controls. RESULTS: A total of 21 patients screened had HyOx (>0.5 mmol/24 h per 1.73 m(2)); they were classified into five groups. Eleven had PH (PH1 in nine and neither PH1 nor PH2 in two). Six had secondary HyOx: two enteric and four dietary. Four could not be classified. Seven patients had concomitant hypercalciuria. Only one of 12 patients was colonised with O formigenes compared to six of 13 controls. CONCLUSIONS: HyOx is an important risk factor for urolithiasis and nephrocalcinosis in children, and can coexist with hypercalciuria. A novel type of PH is proposed. Absence of O formigenes may contribute to HyOx not related to PH1.
机译:目的:调查尿路结石和/或肾钙化病患儿尿草酸盐的排泄,并对高草酸尿症(HyOx)进行分类。方法:总共筛选了106名患者。在草酸盐:肌酐比例增加的人群中,测定了24小时尿草酸盐排泄量。如果怀疑原发性高草酸尿症(PH),则进行肝活检和/或基因组分析。检查了粪便标本中与1型或2型PH(PH1,PH2)无关的HyOx中是否存在甲醛杆菌。结果:总共筛查了21例患者的HyOx(每1.73 m(2)> 0.5 mmol / 24 h);他们分为五个组。十一个人有PH(PH1为九,PH1和PH2都不为二)。六名患有继发性HyOx:两剂肠溶,四剂饮食。无法分类四个。七例伴有高钙尿症。与13个对照组中的6个相比,12个患者中只有1个被O富集基因定植。结论:HyOx是儿童尿路结石和肾钙化的重要危险因素,可与高钙尿症并存。提出了一种新型的PH。缺乏O富集基因可能会导致与PH1无关的HyOx。

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