VEGFR2 rs2305948 多态性与心肌梗死长期预后的关系

A. S. Vorobyov, G. I. Lifshits, E. Zelenskaya, K. Y. Nikolaev
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摘要

目的评估 VEGFR2 rs2305948 多态性与心肌梗死患者长期随访期间心血管事件发生的相关性。 材料与方法研究纳入了 218 例急性心肌梗死(MI)患者,平均年龄为(57.7 ± 9.9)岁(中性 ± 标准差)。经过临床检查和准备后,患者紧急接受了冠状动脉造影术,随后接受了经皮冠状动脉介入治疗(PCI)或冠状动脉旁路移植术(CABG)。所有患者都接受了聚合酶链反应 rs2305948 VEGFR2 等位基因变异的检测。这些患者的长期随访时间为 9 年(2015 年至 2024 年)。 结果结果发现,在长期随访期间,与rs2305948 VEGFR(C/C)患者相比,rs2305948 VEGFR(C/T和T/T)患者更容易出现心血管死亡、急性冠状动脉综合征(ACS)复发、血管再通复发以及综合终点(心血管死亡、急性冠状动脉综合征复发、冠状动脉支架/搭桥血栓形成、急性缺血性脑血管意外、心肌血管再通复发)。通过多变量分析确定,长期随访期间心血管死亡的发生直接受查尔顿合并症指数(p < 0.001)和 rs2305948 VEGFR2(C/T 和 T/T)(p = 0.030)的影响。查尔顿合并症指数(p = 0.014)和 rs2305948 VEGFR2(C/T 和 T/T)(p = 0.034)直接决定了合并终点的发生,而随后使用大剂量他汀类药物进行门诊治疗(p < 0.001)则反之亦然。 结论在长期随访(9年)期间,心肌梗死患者体内存在rs2305948 VEGFR(C/T和T/T)会使心血管死亡的可能性增加2.82倍,综合终点增加2.10倍。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Associations of VEGFR2 rs2305948 polymorphism with long-term prognosis of myocardial infarction
   Aim. To evaluate the associations of VEGFR2 rs2305948 polymorphism with the occurrence of cardiovascular events during long-term follow-up in patients with myocardial infarction.   Material and methods. The study included 218 patients with acute infarction (MI), mean age 57.7 ± 9.9 years (M ± SD). After clinical examination and preparation, patients urgently underwent coronary angiography followed by percutaneous coronary intervention (PCI) or coronary artery bypass grafting (CABG). All patients underwent determination of the rs2305948 VEGFR2 allelic variant by polymerase chain reaction. The duration of long-term follow-up of these patients was 9 years (from 2015 to 2024).   Results. It was determined that during long-term follow-up, patients with rs2305948 VEGFR (C/T and T/T), in contrast to patients with rs2305948 VEGFR (C/C), were more likely to experience cardiovascular death, recurrent acute coronary syndrome (ACS), recurrent revascularization and a combined end point (cardiovascular death, recurrent ACS, coronary stent/bypass thrombosis, acute ischemic cerebrovascular accident, repeated myocardial revascularization). Using multivariate analysis, it was determined that the occurrence of cardiovascular death during long-term follow-up is directly influenced by the Charlton comorbidity index (p < 0.001) and rs2305948 VEGFR2 (C/T and T/T) (p = 0.030). The onset of a combined endpoint is directly determined by the Charlton comorbidity index (p = 0.014) and rs2305948 VEGFR2 (C/T and T/T) (p = 0.034) and vice versa by subsequent outpatient treatment with high doses of statins (p < 0.001).   Conclusions. The presence of rs2305948 VEGFR (C/T and T/T) in patients with MI increases the likelihood of cardiovascular death by 2.82 times and the combined endpoint by 2.10 times during long-term follow-up (9 years).
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