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   metformin and pioglitazone reduce gene expression of inflammatory factors in insulin resistant and hypertrophied adipocytes  
   
نویسنده malekpour-dehkordi zahra ,mohiti-ardekani javad ,naghiaee yousof ,teimourian shahram ,hemati mahdie ,nourbakhsh mitra
منبع iranian journal of diabetes and obesity - 2020 - دوره : 12 - شماره : 4 - صفحه:233 -240
چکیده    Objective: in obesity, chronic low grade inflammation, created by induction of pro-inflammatory markers, causes adipocyte dysfunction in adipose tissue. adipocytes dysfunction is associated with various diseases including insulin resistance and obesity. inobesity, inflammatory factors such as osteopontin (opn), angiopoietin-like protein 2 (angptl2) and transforming growth factor-β (tgf-β) are induced in adipose tissue. metformin and pioglitazone that are used to modulate inflammation, but the relevantmechanism is poorly understood. this study aimed to investigate the effect of metformin and pioglitazone as anti-diabetic drugs, on gene expression of osteopontin, angptl2 and tgf-β as inflammatory factors in insulin resistance and hypertrophied adipocyte in 3t3-l1 cell line model in vitro. materials and methods: in this experimental research, we differentiated3t3-l1 preadipocytes to adipocytes. the adipocytes treated in insulin resistance and hypertrophied conditions withmetformin and pioglitazone and assayed gene expression of opn, angptl2 and tgf-β by real-time pcr. data was analyzed by spss statistic software.results: the results showed that expression of opn, angptl2, and tgf-β were increased significantly over 2-fold (p-value< 0.05) in insulin resistance and hypertrophied adipocytes compared to normaladipocytes. pre- and co-treatment with metformin and pioglitazone led to reduced expression of angptl2 and tgf-β. only metformin significantly reduced the expression of angptl2, tgf-β and opn in hypertrophied adipocyte. conclusion: these results support the proposal that metformin and pioglitazone reduce gene expression of inflammatory factors ininsulin resistant and hypertrophied adipocytes.
کلیدواژه angptl2 ,metformin ,osteopontin ,pioglitazone ,tgf-β
آدرس shahid sadoughi university of medical sciences, faculty of medicine, department of clinical biochemistry, iran, shahid sadoughi university of medical sciences, faculty of medicine, department of clinical biochemistry, iran, shahid sadoughi university of medical sciences, faculty of medicine, department of clinical biochemistry, iran, iran university of medical sciences, faculty of medicine, department of genetics, iran, shahid sadoughi university of medical sciences, faculty of medicine, department of clinical biochemistry, iran, iran university of medical sciences, faculty of medicine, department of biochemistry, iran
پست الکترونیکی nourbakhsh.m@iums.ac.ir
 
     
   
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