The impact of klotho gene polymorphisms on urinary tract stone disease

The impact of klotho gene polymorphisms on urinary tract stone disease

Objectives To investigate the effect of klotho gene and β-glucuronidase activity on stone formation in patients with urinary tract stone disease (UTSD). Methods A total of 103 patients with UTSD and 102 controls with no specific urolithiasis history were enrolled into the study. G395A and C1818T pol...

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Published in:World journal of urology Vol. 34; no. 7; pp. 1045 - 1050
Main Authors: Gürel, Abdullah, Üre, İyimser, Temel, Halide Edip, Çilingir, Oğuz, Uslu, Sema, Celayir, Mehmet Fatih, Aslan, Serap, Başeskioğlu, Ali Barbaros
Format: Journal Article
Language:English
Published: Berlin/Heidelberg Springer Berlin Heidelberg 01-07-2016
Springer Nature B.V
Subjects:
Adolescent
Adult
Aged
Aged, 80 and over
Female
Glucuronidase - genetics
Glucuronidase - metabolism
Humans
Male
Medicine
Medicine & Public Health
Middle Aged
Nephrology
Oncology
Original Article
Polymorphism, Genetic
Prospective Studies
Urinary Calculi - enzymology
Urinary Calculi - genetics
Urology
Young Adult
Urolithiasis
Genetic
Etiology
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Summary:Objectives To investigate the effect of klotho gene and β-glucuronidase activity on stone formation in patients with urinary tract stone disease (UTSD). Methods A total of 103 patients with UTSD and 102 controls with no specific urolithiasis history were enrolled into the study. G395A and C1818T polymorphisms of klotho gene were analyzed with PCR method. Serum levels of calcium and phosphorus and 24-h urine levels of β-glucuronidase activity, calcium and phosphorus levels were measured biochemically. Results A total of 103 of patients were male (50.2 %) and 102 were female (49.8 %) ( p 0.945). Twenty-four-hour urine levels of calcium were significantly higher in UTSD group, whereas no difference was observed in phosphorus levels ( p  < 0.001, p 0.074, respectively). As for the G395A polymorphism, type of GG was significantly higher in the patient group compared to the controls ( p  = 0.02), while GA genotype was significantly higher in the controls ( p  = 0.001). There was no significant difference in F352V and C1818T polymorphism between the patient and control groups. β-glucuronidase activity was slightly lower in the patient group without significance ( p 0.932).When patients with GG genotype and the rest were compared, there were no significant difference in all parameters. Conclusions Any polymorphism altering the function of klotho gene may result with stone formation. We found that there are more GG sequences of G395A gene in patients with UTSD. That may be a polymorphism of klotho gene which results with stone formation. Further studies with more patients should be accomplished which are combining the genetic and epigenetic factors associated with urolithiasis and klotho gene to enlighten the etiology of this disease.
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ISSN:0724-4983
1433-8726
DOI:10.1007/s00345-015-1732-z