Phenotypic variability of cardiovascular manifestations in Marfan Syndrome: Possible role of hyperhomocysteinemia and C677T MTHFR gene polymorphism

doi:10.1016/j.ehj.2003.08.020

European Heart Journal 2003 24(22):2038-2045; doi:10.1016/j.ehj.2003.08.020
Copyright © 2003 by the European Society of Cardiology.

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Clinical research

Phenotypic variability of cardiovascular manifestations in Marfan Syndrome

Possible role of hyperhomocysteinemia and C677T MTHFR gene polymorphism

Betti Giusti^a^,*, Maria Cristina Porciani^a, Tamara Brunelli^a, Lucia Evangelisti^a, Sandra Fedi^a, Gian Franco Gensini^a, Rosanna Abbate^a, Guido Sani^a, Magdi Yacoub^b and Guglielmina Pepe^a

^a Dipartimento di Area Critica Medico Chirurgica, University of Florence, Florence, Italy
^b Department of Cardiothoracic Surgery, National Heart and Lung Institute, Imperial College of Science, Technology and Medicine, Heart Science Centre, Harefield Hospital, Uxbridge, UK

^* Correspondence to: Dr Betti Giusti, PhD, Dipartimento di Area Critica Medico Chirurgica, University of Florence, Viale Morgagni 85, 50134 Florence, Italy. Tel +39-0554279417; Fax +39-0554279418
E-mail address: labctrombosi{at}ao-careggi.toscana.it

Received 13 May 2003; revised 2 August 2003; accepted 21 August 2003

Abstract

Aims The aim of this study was to evaluate (1) homocysteinemiaand the prevalence of the C677T MTHFR polymorphism in Marfanpatients and (2) whether the severity of cardiovascular manifestationsis associated with homocysteinemia and/or C677T polymorphism.

Methods and results We studied 107 patients subdivided intothree subgroups based on the severity of cardiovascular manifestations:(A) no involvement (n=4); (B) mild involvement (n=45); (C) aorticdilatation or aortic dissection (n=58), and 189 controls. Totalhomocysteine (tHcy) was significantly higher in subgroup C thanin subgroup B. In subgroup C patients with dissection tHcy washigher than in those without dissection. In subgroup C the prevalenceof 677T homozygotes was higher, but not significantly, thanin the subgroup B. In patients with dissection the prevalenceof 677T homozygotes was significantly higher than in those withoutdissection and than in subgroup B. In the logistic regressionanalysis, severe cardiovascular manifestations and aortic dissectionin Marfan patients were associated with tHcy plasma levels.

Conclusions Our data indicate an association between the severityof the cardiovascular manifestations, in particular aortic dissection,and elevated tHcy levels. This suggests an important role fortHcy in determining phenotypic variability in Marfan patientsand provides further evidence for the association of homocysteinemiawith the damage of the vascular system.

Key Words: Hyperhomocysteinemia • Marfan syndrome • 5,10-methylenetetrahydrofolate reductase • Aneurysm • Aorta • Risk factors

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