Joint effects of PPARG-C161T (rs3856806) polymorphism and cardiovascular risk factors on restenosis risk after coronary stent implantation

Z. Javadova, Fatih Yanar, E. Aslan, G. Ozkara, Fidan Malikova, Onur Kılıcarslan, O. Ser, Ahmet Yildiz, O. Kucukhuseyin, O. Ozturk, Hülya YILMAZ AYDOĞAN
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Abstract

Abstract Objectives The peroxisome proliferator-activated receptor gamma (PPARG) C161T polymorphism (rs3856806) may be a risk factor for in-stent restenosis (ISR) due to its known associations with type 2 diabetes (T2DM), obesity, and coronary artery disease (CAD). This study aims to investigate the relationship between PPARG-C161T polymorphism and the risk of ISR, considering clinical features. Methods According to the results of coronary angiography, the patients who had undergone drug-eluting stent implantation were categorized into two groups: ISR (n=116) and non-ISR (n=265). The control group consisted of 140 healthy subjects with asymptomatic for CAD or any systemic disease. PPARG-C161T genotypes were determined using the real-time polymerase chain reaction melting curve analysis. Results T2DM, hypertension, and hyperlipidemia were observed as the main clinical features causing non-ISR and ISR. The 161-CC genotype was associated with an increased risk of ISR compared to both controls (p=0.014) and non-ISR patients (p=0.008). This difference remained statistically significant after multivariate analysis for non-ISR patients (p=0.003) but not for the ISR group. The prevalence of hypertension and hyperlipidemia was higher in ISR patients with T2DM than in non-ISR patients with T2DM (p=0.002 and p=0.009, respectively). Multivariate logistic regression analysis in subgroups based on the presence of T2DM showed that hypertension (p<0.001) was associated with ISR in patients with T2DM. Conclusions This study points out the association between the PPARG 161-CC genotype and the risk of ISR, which also means that the PPARG 161-T allele is protective against ISR. However, this effect could be divergent in the presence of the metabolic components of the restenosis phenotype, especially T2DM.
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PPARG-C161T (rs3856806) 多态性和心血管风险因素对冠状动脉支架植入术后再狭窄风险的共同影响
摘要 目的 过氧化物酶体增殖激活受体γ(PPARG)C161T多态性(rs3856806)可能是支架内再狭窄(ISR)的危险因素,因为它与2型糖尿病(T2DM)、肥胖和冠状动脉疾病(CAD)有已知的关联。本研究旨在结合临床特征,探讨 PPARG-C161T 多态性与 ISR 风险之间的关系。方法 根据冠状动脉造影结果,将接受药物洗脱支架植入术的患者分为两组:ISR组(116人)和非ISR组(265人)。对照组由 140 名无 CAD 症状或任何系统疾病的健康受试者组成。PPARG-C161T 基因型通过实时聚合酶链反应熔解曲线分析确定。结果 观察到 T2DM、高血压和高脂血症是导致非 ISR 和 ISR 的主要临床特征。与对照组(P=0.014)和非 ISR 患者(P=0.008)相比,161-CC 基因型与 ISR 风险增加有关。对非 ISR 患者进行多变量分析后,这一差异仍具有统计学意义(p=0.003),但对 ISR 组则没有意义。患有 T2DM 的 ISR 患者的高血压和高脂血症患病率高于患有 T2DM 的非 ISR 患者(分别为 p=0.002 和 p=0.009)。根据是否存在 T2DM 进行分组的多变量逻辑回归分析表明,高血压(p<0.001)与 T2DM 患者的 ISR 相关。结论 本研究指出 PPARG 161-CC 基因型与 ISR 风险之间存在关联,这也意味着 PPARG 161-T 等位基因对 ISR 具有保护作用。然而,如果存在再狭窄表型的代谢成分,尤其是 T2DM,这种效应可能会出现偏差。
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