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Systemic oxidative stress, as measured by urinary allantoin and F(2)-isoprostanes, is not increased in Down syndrome.

Annals of epidemiology (2012-10-16)
Adviye A Tolun, Peter M Scarbrough, Haoyue Zhang, Jane-Ann McKillop, Frances Wang, Priya S Kishnani, David S Millington, Sarah P Young, Dora Il'yasova
RÉSUMÉ

Oxidative stress has been implicated in Down syndrome (DS) pathology. This study compares DS individuals and controls on their urinary levels of allantoin and 2,3-dinor-iPF2α-III; these biomarkers have been previously validated in a clinical model of oxidative stress. Urine samples were collected from 48 individuals with DS and 130 controls. Biomarkers were assayed by ultraperformance liquid chromatography-tandem mass spectrometry, normalized by urinary creatinine concentration. After adjusting for age and gender, mean allantoin levels were lower among DS individuals versus controls (P = .04). The adjusted mean levels of 2,3-dinor-iPF2α-III were similar in DS individuals and controls (P = .7). Our results do not support the hypothesis that DS individuals have chronic systemic oxidative stress.

MATÉRIAUX
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Sigma-Aldrich
Allantoin, ≥98.0% (N)
Supelco
Allantoin, analytical standard
Allantoin, European Pharmacopoeia (EP) Reference Standard