Cardiac and Vascular Hypertrophy in Fabry Disease: Evidence for a New Mechanism Independent of Blood Pressure and Glycosphingolipid Deposition

doi:10.1161/01.ATV.0000209649.60409.38

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Arteriosclerosis, Thrombosis, and Vascular Biology. 2006;26:839-844
Published online before print February 9, 2006, doi: 10.1161/01.ATV.0000209649.60409.38

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(Arteriosclerosis, Thrombosis, and Vascular Biology. 2006;26:839.)
© 2006 American Heart Association, Inc.

Vascular Biology

Cardiac and Vascular Hypertrophy in Fabry Disease

Evidence for a New Mechanism Independent of Blood Pressure and Glycosphingolipid Deposition

Frédéric Barbey; Noureddine Brakch; Ale $s$ Linhart; Nathalie Rosenblatt-Velin; Xavier Jeanrenaud; Salah Qanadli; Beat Steinmann; Michel Burnier; Tomas Palecek; Jan Bultas; Daniel Hayoz

From the Nephrology Department (F.B., M.B.), University Hospital, Lausanne, Switzerland; Department of Vascular Medicine (N.B., N.R.-V., D.H.), University Hospital, Lausanne, Switzerland; Second Department of Internal Medicine (A.L., T.P., J.B.), 1st School of Medicine, Charles University, Prague, Czech Republic; Radiology Department (S.Q.), University Hospital, Lausanne, Switzerland; Cardiology Department (X.J.), University Hospital, Lausanne, Switzerland; Department of Metabolism and Molecular Pediatrics (B.S.), Zürich, Switzerland.

Correspondence to Daniel Hayoz, Department of Vascular Medicine, CHUV 1011-Lausanne, Switzerland. E-mail daniel.hayoz{at}chuv.ch

Objectives— Fabry disease is an X-linked disorder resultingfrom ${alpha}$ -galactosidase A deficiency. The cardiovascular findingsinclude left ventricular hypertrophy (LVH) and increased intima-mediathickness of the common carotid artery (CCA IMT). The currentstudy examined the possible correlation between these parameters.To corroborate these clinical findings in vitro, plasma fromFabry patients was tested for possible proliferative effecton rat vascular smooth muscle cells (vascular smooth musclecell [VSMC]) and mouse neonatal cardiomyocytes.

Methods and Results— Thirty male and 38 female patientswere enrolled. LVH was found in 60% of men and 39% of women.Increased CCA IMT was equally present in males and females.There was a strong positive correlation between LV mass andCCA IMT (r²=0.27; P<0.0001). VSMC and neonatal cardiomyocyteproliferative response in vitro correlated with CCA IMT (r²=0.39;P<0.0004) and LV mass index (r²=0.19; P=0.028), respectively.

Conclusions— LVH and CCA IMT occur concomitantly in Fabrysuggesting common pathogenesis. The underlying cause may bea circulating growth-promoting factor whose presence has beenconfirmed in vitro.

The study examined and confirmed the correlation between 2 cardiovascularfindings in Fabry disease, LVH and CCA IMT. Further in vitroinvestigation confirmed the presence of a circulating growth-promotingfactor that may be at least partially responsible for theseclinical findings.

Key Words: Fabry disease • growth-promoting factor • intima–media thickness • left ventricular hypertrophy

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