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| Item Type: | Article |
|---|---|
| Title: | The E-selectin SER128ARG gene polymorphism and restenosis after successful coronary angioplasty |
| Creators Name: | Rauchhaus, M. and Gross, M. and Schulz, S. and Francis, D.P. and Greiser, P. and Norwig, A. and Weidhase, L. and Coats, A.J.S. and Dietz, R. and Anker, S.D. and Glaser, C. |
| Abstract: | Objectives: Coronary angioplasty remains plagued by the problem of restenosis. Genetic polymorphisms may contribute to the development of restenosis by mediating exaggerated inflammatory responses of the endothelium to angioplasty-induced injury. Background: The serine (Ser)-128-arginine (Arg) gene polymorphism of E-selectin has been implicated in the pathogenesis of coronary artery disease (CAD). We sought to explore whether allelic variants relate to post-angioplasty restenosis. Methods: The 128Arg allele was analyzed by PCR in 101 (derivation study, age 54±1 years, all mean±S.E.M.) and 92 (validation study, age 62±1 years) patients with CAD who underwent successful angioplasty. Results: Restenosis, defined as >50% luminal diameter reduction at the target lesion at follow-up angiography, was found in 54/101 (53%) and 43/92 (47%) patients during follow-up. The 128Arg allele frequency in the derivation study was 10.39% and was 11.96% in the validation study. The 128Arg allele was more prevalent in the restenosis groups (14.81% and 17.44%, respectively) than in the restenosis-free groups (5.32% and 7.14%, respectively, p=0.027 and p=0.031). In multivariate logistic regression, the 128Arg allele emerged as a predictor of restenosis in both studies (p<0.05). There were no differences in the level of soluble E-selectin according to genotype, gender, age (p>0.20), and between patients with restenosis and those without (43.8±3.2 vs. 47.4±3.1 ng/ml, p>0.20). Conclusions: The 128Arg allele of E-selectin may be related to increased endothelial responses to injury, thereby potentially serving as a risk factor for post-angioplasty restenosis in patients with CAD. The development of restenosis remains a problem in patients with CAD. The Ser128Arg polymorphism of E-selectin was analyzed in 101 (derivation) and 92 (validation) CAD patients. Patients with restenosis (54/101 and 43/92) had a higher frequency of the 128Arg allele (14.81 and 17.44%) than those without (5.32%, p=0.027 and 7.14%, p=0.031). In logistic regression, the 128Arg allele emerged as a predictor of restenosis in both studies (p<0.05). The E-selectin 128Arg allele may serve as a risk factor for the development of restenosis. |
| Keywords: | Angioplasty, Cell Adhesion Molecules, E-Selectin, Genetics, Restenosis |
| Source: | International Journal of Cardiology |
| ISSN: | 0167-5273 |
| Publisher: | Elsevier |
| Volume: | 83 |
| Number: | 3 |
| Page Range: | 249-257 |
| Date: | 1 January 2002 |
| Official Publication: | https://doi.org/10.1016/S0167-5273(02)00073-6 |
| PubMed: | View item in PubMed |
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