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a Departments of Clinical and Experimental Medicine, Section of Internal Medicine II
b Vascular Surgery, University of Ferrara, Italy
c Gerontology and Geriatrics, Department of Clinical and Experimental Medicine, University of Perugia, Italy
d Department of Medicine and Aging, University of Chieti, Italy
Renato Fellin, Istituto di Medicina Interna II, Universita' degli Studi, via Savonarola n° 9, 44100 Ferrara, Italy E-mail: flr{at}ifeuniv.it.
Background. Atherosclerosis (ATS) is a common age-related disease of large arteries. The prevalence of older subjects with vascular successful aging (VaSA), defined as the absence of clinical symptoms and instrumental signs of ATS, is low in Western countries. The possible contribution of genetics to the VaSA phenomenon is not known.
Methods. We investigated the distribution of four genetic polymorphisms (angiotensin converting enzyme [ACE], methylenetetrahydrofolate reductase [MTHFR], apolipoprotein E [apo E], and paraoxonase [PON] genes) in 30 subjects with VaSA, 30 subjects with moderate carotid atherosclerosis (ATS group), and 161 controls with a negative history for cardiovascular disease. Clinical examination; ultrasonographic examination of carotid, vertebral, abdominal aortic, iliac, and femoral arteries; and electrocardiogram were performed.
Results. The frequency of PON 192 B allele was lower in VaSA patients (13%) compared with ATS patients (37%) and controls (46%) ( p = .06 and .006, respectively); B/B homozygotes were 27% in the ATS group, 12% in controls, and 0% in the VaSA group. The frequency of the MTHFR thermolable + allele was higher in VaSA (0.51) compared with ATS (0.39) and controls (0.40) (VaSA vs C, p = .006). No differences in the distribution of ACE I/D and apo E alleles emerged between the three groups.
Conclusions. The low prevalence of the PON 192 B allele in the VaSA subjects suggests that this polymorphism might have an important role in VaSA, probably by hydrolyzing lipid peroxides and thus preventing low-density lipoprotein from undergoing the oxidative modification. This finding further supports the oxidative hypothesis of ATS.
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