Prevalence of Fabry Disease in Patients on Dialysis in France

被引:0
作者
Sens, Florence [1 ,2 ]
Guittard, Laure [3 ,4 ]
Knebelmann, Bertrand [5 ]
Moranne, Olivier [6 ]
Choukroun, Gabriel [7 ]
de Precigout, Valerie [8 ]
Couchoud, Cecile [9 ]
Deleruyelle, Isabelle [3 ]
Lancelot, Lea [3 ]
Phuong, Lien Tran Thi [10 ]
Ghafari, Thomas [11 ]
Juillard, Laurent [1 ,2 ]
Germain, Dominique P. [10 ,11 ,12 ]
机构
[1] Hosp Civils Lyon, Hop Edouard Herriot, Serv Nephrol, F-69003 Lyon, France
[2] Univ Claude Bernard Lyon 1, INSERM, UMR 1060, F-69621 Villeurbanne, France
[3] Hosp Civils Lyon, Serv Rech & Epidemiol Clin, Pole Sante Publ, F-69002 Lyon, France
[4] Univ Claude Bernard Lyon, Res Healthcare Performance RESHAPE, INSERM, U1290, F-69373 Lyon, France
[5] Univ Paris, AP HP, Hop Necker, Serv Nephrol, F-75015 Paris, France
[6] Univ Montpellier, Hop Univ Caremeau, Serv Nephrol Dialyse Apherese, IDESP, F-30029 Nimes, France
[7] CHU Amiens, Med Interne Dialyse & Transplantat, Serv Nephrol, F-80054 Amiens, France
[8] CHU Bordeaux, Hop Pellegrin, Serv Nephrol, F-33076 Bordeaux, France
[9] Agence Biomed, Coordinat Natl Reseau Epidemiol & Informat Nephrol, F-93212 Plaine, France
[10] MetabERN European Reference Network, Geneo Referral Ctr Fabry Dis & Lysosomal Dis, F-92380 Garches, France
[11] Paris Saclay Univ, APHP, Div Med Genet, F-92380 Garches, France
[12] Univ Versailles, Div Med Genet, F-78180 Montigny, France
关键词
Fabry disease; dialysis; screening; prevalence; genetic variants; CHRONIC KIDNEY-DISEASE; STAGE RENAL-DISEASE; GALACTOSIDASE-A DEFICIENCY; INFORMATION NETWORK REIN; DRIED BLOOD SPOTS; ALPHA-GALACTOSIDASE; HEMODIALYSIS-PATIENTS; 2-TIER APPROACH; DIAGNOSIS; PLASMA;
D O I
10.3390/ijms251810104
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
Numerous prevalence studies on Fabry disease (FD, OMIM #301500) have been conducted in dialysis populations across the world with variable and controversial results. The FABRYDIAL study aimed to estimate the prevalence of FD in patients aged 18 to 74 years on chronic dialysis in France. This cross-sectional study was conducted in patients undergoing dialysis. One hundred and twenty-four dialysis centers participated. Patients with proven causes of nephropathy unrelated to FD were excluded. Alpha-galactosidase A activity was assayed in men, and both alpha-galactosidase A and lyso-Gb3 were assayed in women from dried blood spots. GLA gene sequencing was performed in case of abnormal values. If a variant was identified, a diagnosis validation committee was consulted for adjudication. Among the 6032 targeted patients, 3088 were included (73.6% of the eligible patients). Biochemical results were available for 2815 (1721 men and 1094 women). A genetic variant of GLA was identified in five patients: a benign c.937G>T/p.(Asp313Tyr) variant in two individuals, a likely benign c.427G>A/(p.Ala143Thr) variant, a likely benign c.416A>G/(p.Asn139Ser) variant, and a pathogenic c.1185dupG/p.Phe396Glyfs variant. Among the screened patients, the prevalence was 0.058% [0.010;0.328] in males, 0% [0.000;0.350] in females, and 0.035% [0.006;0.201] when both genders were pooled. Among all patients aged 18-74 years undergoing dialysis without a previously known cause of nephropathy unlinked to FD, the prevalence was 0.028% [0.006;0.121]. The prevalence of FD in a cohort of French dialysis patients was low. However, considering the prognostic impact of earlier diagnosis, signs of FD should be sought in patients with nephropathies of uncertain etiology.
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