Title of article :
The association between genetic polymorphisms of the interleukin‑10, tumor necrosis factor‑alpha, and annexin A5 gene loci and restenosis after percutaneous coronary angioplasty and stenting
Author/Authors :
Hashemi, Mohammad Department of Cardiology - Faculty of Medicine - Chamran Hospital - Isfahan University of Medical Sciences , Baktashian, Mojtaba Student Research Committee - Faculty of Medicine - Mashhad University of Medical Sciences , Hosseinpour Moghaddam, Kiana Department of Biology - Faculty of Sciences - Ferdowsi University of Mashhad , Salehi, Mansoor Department of Genetics - Faculty of Medicine and Genetics Laboratory - Al-Zahra Medical and Educational Center - Isfahan University of Medical Sciences , Saffar Soflaei, Sara Student Research Committee - Faculty of Medicine - Mashhad University of Medical Sciences , Ferns, Gordon Division of Medical Education - Brighton and Sussex Medical School - University of Brighton, UK , Pasdar, Alireza Department of Modern Sciences and Technologies - Faculty of Medicine - Mashhad University of Medical Sciences , Ghayour Mobarhan, Majid Metabolic Syndrome Research Center - School of Medicine - Mashhad University of Medical Sciences
Abstract :
Background: Advances in the technology for percutaneous coronary angioplasty, such as coated stents, have reduced its complications, but restenosis remains an important clinical problem. The factors associated with an increased risk of restenosis include diabetes mellitus and multiple coronary artery disease. It is also possible that genetic factors play a role in restenosis although there are little data on this. We have investigated the association of three genetic markers of genes involved in inflammation leading to restenosis. Materials and Methods: In this case–control study, 306 unrelated Iranian patients who were thought to have restenosis on clinical grounds were investigated. Based on the results of angiography, 104 patients were found to have >50% stenosis within an implanted stent, and these were allocated to the in‑stent restenosis (ISR) group; 202 patients with no in‑stent stenosis or stenosis ≤50% were allocated to the non‑ISR (NISR) group. Demographic data were collected from medical records. Biochemical parameters were measured using routine methods. Genotypes of the interleukin‑10 (IL‑10), annexin A5 (AnxA5), and tumor necrosis factor‑alpha (TNFα) loci were determined using real‑time polymerase chain reaction and a high‑resolution melting assay. Results: Fasting blood glucose, serum triglycerides, and serum high‑sensitivity C‑reactive protein (hs‑CRP) concentrations were higher in the ISR group than in the NISR group (P < 0.05), and a history of diabetes mellitus was significantly related to the presence of restenosis (P < 0.001). There were no significant differences in the frequency of the genetic polymorphisms of IL‑10, AnxA5, and TNFα genes and the presence of ISR. Conclusion: After adjustment for clinical variables, the genetic polymorphisms at the IL‑10, TNFα, and ANXA5 gene loci do not appear to be risk factors for >50% ISR in our population. However, our data suggested a significant association between diabetes mellitus, serum hs‑CRP, stent type, and restenosis.
Keywords :
Annexin A5 , in‑stent restenosis , interleukin‑10 , single‑nucleotide polymorphism , tumor‑necrotizing factor
Journal title :
Journal of Research in Medical Sciences
