| Literature DB >> 33867715 |
Nuttikarn Nokkaew1,2, Podsawee Mongkolpathumrat1,2, Ruttanapong Junsiri2, Supawit Jindaluang2, Nichagron Tualamun2, Niya Manphatthanakan2, Nareumon Saleesee2, Marisa Intasang2, Jantira Sanit1,2, Punyanuch Adulyaritthikul1,2, Kantapich Kongpol1,2, Sarawut Kumphune1,2,3, Nitirut Nernpermpisooth1,2,4.
Abstract
Microvascular and macrovascular diseases are the main causes of morbidity in type 2 diabetes patients through chronic hyperglycaemic condition via oxidative stress and inflammation. Reactive oxygen species (ROS) activate p38 MAPK phosphorylation and inflammation which enhances protein modification by carbonylation. The use of metformin and a p38 MAPK inhibitor is hypothesised to reduce ROS production and inflammation but effects of metformin and p38 MAPK inhibitor (SB203580) on ROS production and inflammation in vascular type 2 diabetes mellitus non-obese (T2DM) have not been investigated. The Goto-Kakizaki rat T2DM model was divided into three groups as T2DM, T2DM treated with 15 mg/kg bw metformin and T2DM treated with 2 mg/kg bw SB203580 for 4 weeks. Rat aortas were isolated and protein carbonyl (PC) contents were measured by spectrophotometric DNPH assay. Aortic IL-1ß level was determined by ELISA. Results showed that aortic PC contents in the T2DM group were significantly higher than in non-diabetic rats. Treatment with metformin or SB203580 significantly reduced PC contents while only metformin significantly reduced IL-1ß levels. Findings indicated that metformin reduced ROS production and inflammation in diabetic vessels and possibly reduce vascular complications in non-obese T2DM. © Association of Clinical Biochemists of India 2019.Entities:
Keywords: Inflammation; Metformin; Protein carbonyl; SB203580; Type 2 diabetes mellitus; Vascular complications
Year: 2019 PMID: 33867715 PMCID: PMC7994467 DOI: 10.1007/s12291-019-0815-9
Source DB: PubMed Journal: Indian J Clin Biochem ISSN: 0970-1915