[No authors listed]
BACKGROUND:ACS (acute coronary syndrome), a subgroup of coronary artery disease (CHD), is a leading cause of death worldwide. Reports shown the association between methylation and CHD, while the abnormal expression of C1QTNF1 (C1q and tumor necrosis factor related protein 1) in CHD patients, but the underlying mechanisms are still unclear. OBJECTIVE:To analyze the methylation of CpG sites of C1QTNF1 in ACS patients. METHODS:Peripheral blood samples were collected from healthy controls and ACS patients. The methylation of total C1QTNF1, promoter sequence and CpG sites of C1QTNF1 were measured using methylation detection kits. The outcomes were compared between patients and controls based on gender, clinical classification and clinical stages. RESULTS:The promoter sequences from 37 ACS patients and 20 controls indicate that the methylation rate of C1QTNF1 was significantly lower in male patients compared to healthy controls at +â63 CpG sites (pâ=â0.03). Whereas, the methylation rate of C1QTNF1 in female patients was significantly lower than female health controls at - 89, +â39 and +â167 CpG sites (pâ=â0.021, 0.042, 0.021). In addition, the methylation rate of C1QTNF1 was significantly higher in male patients than female patients at - 89, - 41 and +â39 CpG sites (pâ=â0.011, 0.043, 0.006). Moreover, the methylation rate significantly decreased at - 24 sites (pâ=â0.021), but it significantly increased at - 14 site (pâ=â0.048) in patients with UA, compared to patients with STEMI (ST-segment elevation myocardial infarction). CONCLUSIONS:There were significant differences in the methylation rateâ+â63 CpG sites between controls and male ACS patients. The -â14 site methylation increased in patients with UA, compared to patients with STEMI.
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