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Predictors of Fabry disease in patients with hypertrophic cardiomyopathy: How to guide the diagnostic strategy? - 16/08/20

Doi : 10.1016/j.ahj.2020.04.006 
Olga Azevedo, MD a, b, c, , Nuno Marques, MD d, e, f, Liliana Reis, MD g, Inês Cruz, MD h, Nuno Craveiro, MD i, Hugo Antunes, MD j, Carolina Lourenço, MD k, Renata Gomes, MD l, Rui Azevedo Guerreiro, MD m, Ricardo Faria, MD n, Fernando Sá, MD o, Rui Lima, MD p, Paulo Gaspar, PhD q, r, Rui Faria, MD s, Gabriel Miltenberger-Miltenyi, PhD b, c, t, Nuno Sousa, MD, PhD b, c, Damião Cunha, MD, PhD b, c

On behalf of the group of investigators

a Cardiology Department, Reference Center on Lysosomal Storage Disorders, Hospital Senhora da Oliveira, Guimarães, Portugal, member of the European Reference Network on Hereditary Metabolic Disorders (MetabERN) 
b Life and Health Sciences Research Institute (ICVS), School of Medicine, University of Minho, Braga, Portugal 
c ICVS/3Bs PT Government Associate Laboratory, Braga/Guimarães, Portugal 
d Cardiology Department, Centro Hospitalar Universitário do Algarve, Faro, Portugal 
e Algarve Biomedical Center, Faro, Portugal 
f Biomedical Science and Medicine Department, Algarve University, Faro, Portugal 
g Cardiology Department, Centro Hospitalar Universitário de Coimbra, Coimbra, Portugal 
h Cardiology Department, Hospital Garcia de Orta, Almada, Portugal 
i Cardiology Department, Hospital de Santarém, Santarém, Portugal 
j Cardiology Department, Centro Hospitalar de Tondela e Viseu, Viseu, Portugal 
k Cardiology Department, Centro Hospitalar do Tâmega e Sousa, Penafiel, Portugal 
l Cardiology Department, Hospital de Santo Espírito, Terceira, Portugal 
m Cardiology Department, Hospital do Espírito Santo, Évora, Portugal 
n Cardiology Department, Centro Hospitalar Médio Ave, Vila Nova de Famalicão, Portugal 
o Cardiology Department, Centro Hospitalar Universitário de Leiria, Leiria, Portugal 
p Cardiology Department, Unidade Local de Saúde do Alto Minho, Viana do Castelo, Portugal 
q Organelle Biogenesis & Function Group, Instituto de Investigação e Inovação em Saúde (I3S), Porto, Portugal 
r Institute of Molecular and Cell Biology (IBMC), Universidade do Porto, Porto, Portugal 
s Communication and Society Research Centre, University of Minho, Braga, Portugal 
t Genetics Department, Reference Center on Lysosomal Storage Disorders, Hospital Senhora da Oliveira, Guimarães, Portugal, member of the European Reference Network on Hereditary Metabolic Disorders (MetabERN) 

Reprint requests: Dr. Olga Azevedo, Cardiology Department, Reference Center on Lysosomal Storage Disorders, Hospital Senhora da Oliveira – Guimarães, Rua dos Cutileiros – Creixomil, 4835-044 Guimarães, Portugal.Cardiology Department, Reference Center on Lysosomal Storage DisordersHospital Senhora da Oliveira – Guimarães, Rua dos Cutileiros – CreixomilGuimarães4835-044Portugal

Abstract

Background

Fabry disease (FD) is a treatable cause of hypertrophic cardiomyopathy (HCM). We aimed to determine the independent predictors of FD and to define a clinically useful strategy to discriminate FD among HCM.

Methods

Multicenter study including 780 patients with the ESC definition of HCM. FD screening was performed by enzymatic assay in males and genetic testing in females. Multivariate regression analysis identified independent predictors of FD in HCM. A discriminant function analysis defined a score based on the weighted combination of these predictors.

Results

FD was found in 37 of 780 patients with HCM (4.7%): 31 with p.F113L mutation due to a founder effect; and 6 with other variants (p.C94S; p.M96V; p.G183V; p.E203X; p.M290I; p.R356Q/p.G360R). FD prevalence in HCM adjusted for the founder effect was 0.9%. Symmetric HCM (OR 3.464, CI95% 1.151-10.430), basal inferolateral late gadolinium enhancement (LGE) (OR 10.677, CI95% 3.633-31.380), bifascicular block (OR 10.909, CI95% 2.377-50.059) and ST-segment depression (OR 4.401, CI95% 1.431-13.533) were independent predictors of FD in HCM. The score ID FABRY-HCM [−0.729 + (2.781xBifascicular block) + (0.590xST depression) + (0.831xSymmetric HCM) + (2.130xbasal inferolateral LGE)] had a negative predictive value of 95.8% for FD, with a cut-off of 1.0, meaning that, in the absence of both bifascicular block and basal inferolateral LGE, FD is a less probable cause of HCM, being more appropriate to perform HCM gene panel than targeted FD screening.

Conclusion

FD prevalence in HCM was 0.9%. Bifascicular block and basal inferolateral LGE were the most powerful predictors of FD in HCM. In their absence, HCM gene panel is the most appropriate step in etiological study of HCM.

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Vol 226

P. 114-126 - août 2020 Retour au numéro
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