Association study of the I/D polymorphism and plasma angiotensin-converting enzyme (ACE) as risk factors for stent restenosis

Author:

RIBICHINI Flavio1,FERRERO Valeria1,MATULLO Giuseppe23,FEOLA Mauro4,VADO Antonello4,CAMILLA Terenzio5,GUARRERA Simonetta2,CARTURAN Sonia2,VASSANELLI Corrado1,USLENGHI Eugenio4,PIAZZA Alberto2

Affiliation:

1. Division of Cardiology, Universita' del Piemonte Orientale, Ospedale Maggiore della Carita', Novara, Italy

2. Department of Genetics, Biology and Biochemistry, Universita' di Torino, Villa Gualino, Torino, Italy

3. I.S.I. (Institute for Scientific Exchange) Foundation, Villa Gualino, Torino, Italy

4. Department of Cardiology and Cardiovascular Surgery, Ospedale Santa Croce, Cuneo, Italy

5. Laboratory of Biochemistry, Ospedale Santa Croce, Cuneo, Italy

Abstract

The ID (insertion/deletion) polymorphism of the ACE (angiotensin-converting enzyme) gene controls plasma ACE levels. Both have been correlated with ISR (in-stent restenosis) in preliminary analyses, but not confirmed in larger studies. In the present study, baseline and 6-month quantitative coronary analysis were performed in 897 patients who had stent implantation and the ID polymorphism genotyped. Plasma ACE levels were measured in 848 patients (95%). Restenosis rates among genotypes were 31.2% DD, 25.5% ID and 28.8% II (not significant). Plasma ACE levels were significantly higher in restenotic patients compared with patients without restenosis (30.7±18.6 units/l compared with 22.8±12.8 units/l; P=0.0001) and a strong independent predictor of ISR [OR (odds ratio)=3.70; 95% CI (confidence interval), 2.40–5.71; P<0.0001], except in diabetics. In the subgroup of diabetics and patients with AMI (acute myocardial infarction), the DD genotypes actually had a lower risk of ISR than the II genotypes (diabetics, OR=0.16; 95% CI, 0.04–0.69; P=0.014; and patients with AMI, OR=0.21; 95% CI, 0.061–0.749; P=0.016). After exclusion of diabetics and patients with AMI, ISR rates for genotypes in 632 patients were 31.7% DD, 24.3% ID and 17.6% II (P=0.02; DD compared with non-DD OR=1.57; 95% CI, 1.09–2.25). The association between the D allele and ISR observed in selected populations does not hold with a larger sample size. Other than sample size, clinical variables can modulate the association between ID polymorphism and ISR. Plasma ACE level is a risk factor for ISR, independently of the ID genotype.

Publisher

Portland Press Ltd.

Subject

General Medicine

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