Paraoxnase1 Gene Polymorphism in Childhood Idiopathic Nephrotic Syndrome

Paraoxonase1 (PON1) is a serum enzyme bound to high-density lipoproteins with antioxidant properties. Molecular studies of PON1 revealed 2 polymorphic sites at amino acids 55 and 192 resulting in 2 different allozymes, the L and M-genotype at residue 55 and A and B at site 192, respectively. We have...

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Bibliographic Details
Published inNephron (2015) Vol. 132; no. 2; p. 137
Main Authors Al-Eisa, Amal A, Sukumaran, Vazhappilly J, Haider, Mohammad Z
Format Journal Article
LanguageEnglish
Published Switzerland 01.01.2016
Subjects
Alleles
Aryldialkylphosphatase - genetics
Child
Child, Preschool
DNA - genetics
Female
Gene Frequency
Genotype
Humans
Incidence
Infant
Kidney Function Tests
Kuwait - epidemiology
Male
Nephrosis, Lipoid - genetics
Nephrotic Syndrome - epidemiology
Nephrotic Syndrome - genetics
Nephrotic Syndrome - pathology
Polymorphism, Genetic - genetics
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Summary:Paraoxonase1 (PON1) is a serum enzyme bound to high-density lipoproteins with antioxidant properties. Molecular studies of PON1 revealed 2 polymorphic sites at amino acids 55 and 192 resulting in 2 different allozymes, the L and M-genotype at residue 55 and A and B at site 192, respectively. We have studied the association between PON1 gene polymorphisms and the minimal change nephrotic syndrome/focal segmental glomerulosclerosis (MCNS/FSGS) types of idiopathic nephrotic syndrome (INS) in Kuwaiti Arab children. The PON1 gene, 55 and 192 polymorphisms were analyzed in 50 children with INS (32 MSCN, 18 FSGS) and compared to 50 controls. Serum creatinine, albumin and lipids were measured in all subjects. The LL genotype was detected in 50% of the INS patients compared to 48% of controls (p = 0.84). The heterozygous LM genotype was detected in 42% of INS patients compared 36% of controls (p = 0.68). The MM-genotype was detected in 8% of INS patients and 16% of controls (p = 0.35). The L-allele frequency in its homozygous and heterozygous forms was found in 71% of INS patients compared to 66% controls (p = 0.54). The L-allele frequency (LM and LL) was significantly higher in FSGS compared to MCNS patients (p = 0.0001) and when compared to controls (p = 0.0007). All patients and controls had the AA form of the 192 PON1 gene polymorphism. Our data demonstrate a strong association between the L-allele of PON1 gene 55 polymorphism with FSGS in Kuwaiti Arab children with INS. PON1 genotyping can help in the early prediction of FSGS, which might guide clinicians to a better therapeutic approach.
ISSN:2235-3186
DOI:10.1159/000442998