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Nitrosylation: An adverse factor in Uremic Hemolytic Syndrome. Antitoxin effect of Ziziphus mistol Griseb
Institution:1. Institute of Soil and Water Conservation, Northwest A&F University, Yangling 712100, China;2. College of Natural Resources and Environment, Northwest A&F University, Yangling 712100, China;3. Key Laboratory of Plant Nutrition and the Agri-environment in Northwest China, Ministry of Agriculture, Yangling 712100, China;4. College of Forestry, Northwest A&F University, Yangling 712100, China;5. Department of Agriculture and Rural Development of Lao Cai, Lao Cai City 330100, Vietnam;1. Institute of Low Temperature and Structure Research, 2 Okólna str., 50-422 Wroc?aw, Poland;2. Department of Bioorganic Chemistry, Institute of Chemistry and Food Technology, Faculty of Production Engineering, Wroc?aw University of Economics and Business, 118/120 Komandorska str., 53-345 Wroc?aw, Poland
Abstract:Toxins of Escherichia coli (STEC) causing Uremic Hemolytic Syndrome (UHS) generate oxidative stress in human blood with more production of nitric oxide (NO) than reactive oxygen species (ROS). Shiga toxin (Stx) together with the hemolysin (Hly) increased lipid oxidation, as evaluated by malondialdehyde MDA and oxidation of proteins. The addition of Ziziphus mistol Griseb extracts decreased NO, ROS, MDA and simultaneously caused an increase in the degradation of oxidized proteins to advanced oxidation protein products (AOPPs) in controls and samples with toxins. Furthermore, the nitrosylated proteins/AOPP ratio was reduced, due to the increase of AOPP. Z. mistol Griseb extracts exhibited a high proportion of polyphenols and flavonoids, with evident correlation with ferrous reduction antioxidant potential (FRAP). The plasma of eight children with UHS showed oxidative stress and NO stimulus, comparable to the effect of toxins during the assays in vitro. UHS children presented high levels of nitrosylated proteins respect to control children of similar age. Although the degradation of oxidized proteins to AOPP rose in UHS children, the nitrosylated proteins/AOPP rate increased as a consequence of the elevated nitrosative stress observed in these patients.
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