Affiliation:
1. Department of Clinical Studies, New Bolton Center University of Pennsylvania School of Veterinary Medicine Kennett Square Pennsylvania USA
2. Department of Pathobiology, New Bolton Center University of Pennsylvania School of Veterinary Medicine Kennett Square Pennsylvania USA
Abstract
AbstractBackgroundEight‐hydroxy‐2′‐deoxyguanosine (8‐OHdG), a biomarker of oxidative damage evaluated in human neurodegenerative disease, has potential to correlate with postmortem diagnosis of neuroaxonal dystrophy/degenerative myeloencephalopathy (NAD/DM) in horses.HypothesisWe hypothesized that 8‐OHdG will be higher in CSF and serum from NAD/DM horses compared with horses with other neurologic diseases (CVSM, EPM) and a control group of neurologically normal horses. We also hypothesized that 8‐OHdG will be higher in CSF compared with serum from NAD/DM horses.AnimalsFifty client‐owned horses with postmortem diagnoses: 20 NAD/DM, 10 CVSM, 10 EPM, and 10 control horses. Serum and CSF samples were obtained between November 2010 and March 2022.MethodsCase‐control study using biobanked samples was performed and commercial competitive ELISA kit (Highly Sensitive 8‐OHdG Check ELISA) utilized. Concentration of 8‐OHdG was quantitated in both CSF and serum and compared between groups.ResultsNo correlation was established between the measures of 8‐OHdG in serum and CSF and group. CSF median [8‐OHdG] for NAD/DM was 169.9 pg/mL (IQR25‐75: 67.18‐210.6), CVSM 157.1 pg/mL (IQR25‐75: 132.1‐229.1), EPM 131.4 pg/mL (IQR25‐75: 102.1‐193.2), and control 149.8 pg/mL (IQR25‐75: 113.3‐196.4). Serum median [8‐OHdG] for NAD/DM was 130 pg/mL (IQR25‐75: 51.73‐157.2), CVSM 125.8 pg/mL (IQR25‐75: 62.8‐170.8), EPM 120.6 pg/mL (IQR25‐75: 87.23‐229.7), and control 157.6 pg/mL (IQR25‐75: 97.15‐245.6). Poisson regression analysis showed no difference established once confounding variables were considered.ConclusionsEight‐OHdG did not aid in antemortem diagnosis of NAD/DM in this cohort of horses. At the time of diagnosis horses with NAD/DM do not have ongoing oxidative stress.
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