the relation between enos −786 c/t, 4 a/b, mmp-13 rs640198 g/t, eotaxin 426 c/t, −384 a/g, and 67 g/a polymorphisms and long-term outcome in patients with coronary artery disease

the relation between enos −786 c/t, 4 a/b, mmp-13 rs640198 g/t, eotaxin 426 c/t, −384 a/g, and 67 g/a polymorphisms and long-term outcome in patients with coronary artery disease

;Vladimír Kincl;Jan Máchal;Adéla Drozdová;Roman Panovský;Anna Vašků
international journal of psychology : journal international de psychologie 2015 Vol. 2015 pp. -
109
kincl2015diseasethe

Abstract

Aim. The purpose of this study is to determine the association between eotaxin 426 C/T, −384 A/G, 67 G/A, eNOS −786 T/C, 4 a/b, and MMP-13 rs640198 G/T and prognosis of patients with known CAD. Methods. From total of 1161 patients referred to coronary angiography, 532 patients with angiographically confirmed CAD were selected. Their long-term outcome was followed up using hospital database. Subsequent events were assessed in this study: death or combined endpoint-myocardial infarction, unstable angina pectoris, revascularization, heart failure hospitalization, and cardioverter-defibrillator implantation. Results. The multivariate Cox regression model identified age, smoking, and 3-vessel disease as significant predictors of all-cause death. Further analysis showed that eotaxin 67 G/A (GA + AA versus GG) and eotaxin −384 A/G (GG versus GA + AA) were significant independent prognostic factors when added into the model: HR (95% CI) 2.81 (1.35–5.85), p=0.006; HR (95% CI) 2.63 (1.19–5.83), p=0.017; eotaxin −384 A/G was significantly associated with the event-free survival, but it did not provide the prognostic information above the effect of two- or three-vessel disease. Conclusion. The A allele in eotaxin 67 G/A polymorphism is associated with worse survival in CAD patients.

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