Cardiac involvement in Anderson-Fabry Disease, a rare X-linked genetic lysosomal storage disorder, is common and more than 50% of patients developsa concentric non-obstructive left ventricle hypertrophy.Aim: Aim of study was to identify early signs of myocardial involvement in patients with Fabry Disease without hypertrophy, using 2D Speckle TrackingEchocardiography to evaluate the Left Ventricle Longitudinal Strain (GLS).We evaluated Echocardiograms of 21 patients (7 males, 14 females) with diagnosis of Fabry Disease. For this study we reported the values of the LV massindexed by body surface area (LVMi), E wave of mitral flow, the systolic (S') and early diastolic myocardial velocity (E') of tissue Doppler at mitral annulus,E/E' ratio and GLS. Patients were grouped according to the presence or absence of LV hypertrophy in two groups: with LVMi >115 g/m2 (LVH) and with LVMi<=115 g/m2 (noLVH); the data were compared to normal group (N) matched for age and BSA. LVH pts (2M-3F, 53 ± 9y) showed: Enzyme activity 1,54 ± 1,98;LVMi g/m2150 ± 23,6; E cm/s 70,4 ± 23,7 (vs. p<0,196); S'cm/s 5,4 ± 1,1 (vs. p<0,001); E' 5,2 ± 2,7 (vs. p<0,001); E/E' 16,96 ± 11,8 (vs. p<0,0005);GLS% -11,7 ± 5,4. (vs. p<0,001).NoLVH pts (5M-11F, 33 ± 19y) showed: Enzyme activity 3,43 ± 3,03; LVMi g/m270 ± 16,4 (vs. p<0,719); E cm/s 82,1 ±29,6 (vs. p<0,807); S' cm/s 7,2 ± 1,6 (vs. p<0,001); E' 12 ± 4,1 (vs. p<0,204); E/E' 8 ± 3 (vs. p<0,0005); GLS% - 18,4 ± 2,8 (vs. p<0,02). Our study showsthat even in patients without hypertrophy, then in the pre-clinical stage, the longitudinal ventricle function, expressed by GLS is already precociously altered.
Myocardial dysfunction in Anderson-Fabry disease (AFD) without ventricular hypertrophy
Margherita StefaniaRodolico;Giovanni Duro
2016
Abstract
Cardiac involvement in Anderson-Fabry Disease, a rare X-linked genetic lysosomal storage disorder, is common and more than 50% of patients developsa concentric non-obstructive left ventricle hypertrophy.Aim: Aim of study was to identify early signs of myocardial involvement in patients with Fabry Disease without hypertrophy, using 2D Speckle TrackingEchocardiography to evaluate the Left Ventricle Longitudinal Strain (GLS).We evaluated Echocardiograms of 21 patients (7 males, 14 females) with diagnosis of Fabry Disease. For this study we reported the values of the LV massindexed by body surface area (LVMi), E wave of mitral flow, the systolic (S') and early diastolic myocardial velocity (E') of tissue Doppler at mitral annulus,E/E' ratio and GLS. Patients were grouped according to the presence or absence of LV hypertrophy in two groups: with LVMi >115 g/m2 (LVH) and with LVMi<=115 g/m2 (noLVH); the data were compared to normal group (N) matched for age and BSA. LVH pts (2M-3F, 53 ± 9y) showed: Enzyme activity 1,54 ± 1,98;LVMi g/m2150 ± 23,6; E cm/s 70,4 ± 23,7 (vs. p<0,196); S'cm/s 5,4 ± 1,1 (vs. p<0,001); E' 5,2 ± 2,7 (vs. p<0,001); E/E' 16,96 ± 11,8 (vs. p<0,0005);GLS% -11,7 ± 5,4. (vs. p<0,001).NoLVH pts (5M-11F, 33 ± 19y) showed: Enzyme activity 3,43 ± 3,03; LVMi g/m270 ± 16,4 (vs. p<0,719); E cm/s 82,1 ±29,6 (vs. p<0,807); S' cm/s 7,2 ± 1,6 (vs. p<0,001); E' 12 ± 4,1 (vs. p<0,204); E/E' 8 ± 3 (vs. p<0,0005); GLS% - 18,4 ± 2,8 (vs. p<0,02). Our study showsthat even in patients without hypertrophy, then in the pre-clinical stage, the longitudinal ventricle function, expressed by GLS is already precociously altered.File | Dimensione | Formato | |
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