- 作者:Blanka ; Stiburkovaa ; ; bstib@lf1.cuni.cz ; Jakub ; Krijta ; Petr ; Vyletala ; ; b ; Josef ; Bartla ; Eva ; Gerhatovac ; Martin ; Korinekd ; Ivan ; Sebestaa ; ; e
- 关键词:Xanthinuria ; Xanthine dehydrogenase/oxidase ; Hypouricemia
- 刊名:Clinica Chimica Acta
- 出版年:2012
- 出版时间:18 January 2012
- 年:2012
- 卷:413
- 期:1-2
- 页码:93-99
- 全文大小:393 K
Background
The article describes the clinical, biochemical, enzymological and molecular genetics findings in two patients from two families with xanthinuria type I.Methods
Biochemical analysis using high performance liquid chromatography, allopurinol loading test and analysis of xanthine oxidase activity in plasma and of uromodulin excretion in urine were performed. Sequencing analysis of the xanthine dehydrogenase gene and the haplotype and statistical analyses of consanguinity were performed.
Results
Probands showed extremely low concentrations of uric acid, on seven occasions under the limit of detection. The concentration of uric acid in 38-year-old female was 15 ¦Ìmol/L in serum and 0.04 mmol/L in urine. Excretion of xanthine in urine was 170 mmol/mol creatinine. The concentration of uric acid in 25-year-old male was 0.03 mmol/L in urine. Excretion of xanthine in urine was 141 mmol/mol creatinine. The allopurinol loading test confirmed xanthinuria type I. The xanthine oxidase activities in patients were 0 and 0.4 pmol/h/mL of plasma. We found three nonsense changes: p.P214QfsX4 and unpublished p.R825X and p.R881X.
Conclusions
We found two nonconsanguineous compound heterozygotes with xanthinuria type I caused by three nonsense changes. The methods used did not confirm consanguinity in the probands, thus there might be an unconfirmed biological relationship or mutational hotspot.