Metabolic interactions of AGE inhibitor pyridoxamine and antioxidant α-lipoic acid following 22 weeks of treatment in obese Zucker rats

EM Muellenbach, CJ Diehl, MK Teachey, KA Lindborg… - Life sciences, 2009 - Elsevier
EM Muellenbach, CJ Diehl, MK Teachey, KA Lindborg, O Hasselwander, M Matuschek…
Life sciences, 2009Elsevier
AIMS: The advanced glycation end product inhibitor pyridoxamine (PYR) and the antioxidant
α-lipoic acid (LA) interact to ameliorate insulin resistance in obese Zucker rats following
short-term (6-week) treatment. This study was designed to ascertain whether these unique
interactive effects of PYR and LA remain manifest following longer-term (22-week) treatment.
MAIN METHODS: Female obese Zucker rats received vehicle (OV), PYR (OP, 60 mg/kg
body wt), racemic LA (rac-LA; OM, 92 mg/kg), the R-(+)-enantiomer of LA (R-LA; OR, 92 …
AIMS
The advanced glycation end product inhibitor pyridoxamine (PYR) and the antioxidant α-lipoic acid (LA) interact to ameliorate insulin resistance in obese Zucker rats following short-term (6-week) treatment. This study was designed to ascertain whether these unique interactive effects of PYR and LA remain manifest following longer-term (22-week) treatment.
MAIN METHODS
Female obese Zucker rats received vehicle (OV), PYR (OP, 60 mg/kg body wt), racemic LA (rac-LA; OM, 92 mg/kg), the R-(+)-enantiomer of LA (R-LA; OR, 92 mg/kg), or combined treatments with PYR and rac-LA (OPM) or PYR and R-LA (OPR), daily for 22 weeks.
KEY FINDINGS
Individual and combined treatments with PYR, rac-LA, and R-LA significantly (p<0.05) inhibited skeletal muscle protein carbonyls (28–36%), a marker of oxidative damage, and triglyceride levels (21–51%). Plasma free fatty acids were reduced in OM (9%), OR (11%), and OPM (16%), with the greatest decrease (26%) elicited in OPR. HOMA-IR, an index of fasting insulin resistance, was decreased in OP (14%) and OPM (17%) groups, with the greatest inhibition (22%) in OPR. Insulin resistance (glucose–insulin index) was lowered (20%) only in OPR. Insulin-mediated glucose transport in isolated skeletal muscle was improved in OM (34%), OR (33%), OPM (48%) and OPR (31%) groups.
SIGNIFICANCE
Important interactions between PYR and LA for improvements in glucose and lipid metabolism in the female obese Zucker rat are manifest following a 22-week treatment regimen, providing further evidence for targeting oxidative stress as a strategy for reducing insulin resistance.
Elsevier
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