PT - JOURNAL ARTICLE AU - Doheny, Dana AU - Srinivasan, Ram AU - Pagant, Silvere AU - Chen, Brenden AU - Yasuda, Makiko AU - Desnick, Robert J TI - Fabry Disease: prevalence of affected males and heterozygotes with pathogenic <em>GLA</em> mutations identified by screening renal, cardiac and stroke clinics, 1995–2017 AID - 10.1136/jmedgenet-2017-105080 DP - 2018 Apr 01 TA - Journal of Medical Genetics PG - 261--268 VI - 55 IP - 4 4099 - http://jmg.bmj.com/content/55/4/261.short 4100 - http://jmg.bmj.com/content/55/4/261.full SO - J Med Genet2018 Apr 01; 55 AB - Background Fabry Disease (FD), an X linked lysosomal storage disease due to pathogenic α-galactosidase A (GLA) mutations, results in two major subtypes, the early-onset Type 1 ‘Classic’ and the Type 2 ‘Later-Onset’ phenotypes. To identify previously unrecognised patients, investigators screened cardiac, renal and stroke clinics by enzyme assays. However, some screening studies did not perform confirmatory GLA mutation analyses, and many included recently recognised ‘benign/likely-benign’ variants, thereby inflating prevalence estimates.Methods Online databases were searched for all FD screening studies in high-risk clinics (1995–2017). Studies reporting GLA mutations were re-analysed for pathogenic mutations, sex and phenotype. Phenotype-specific and sex-specific prevalence rates were determined.Results Of 67 studies, 63 that screened 51363patients (33943M and 17420F) and provided GLA mutations were reanalysed for disease-causing mutations. Of reported GLA mutations, benign variants occurred in 47.9% of males and 74.1% of females. The following were the revised prevalence estimates: among 36820 (23954M and 12866F) haemodialysis screenees, 0.21% males and 0.15% females; among 3074 (2031M and 1043F) renal transplant screenees, 0.25% males and no females; among 5491 (4054M and 1437F) cardiac screenees, 0.94% males and 0.90% females; and among 5978 (3904M and 2074F) stroke screenees, 0.13% males and 0.14% females. Among male and female screenees with pathogenic mutations, the type 1 Classic phenotype was predominant (~60%), except more male cardiac patients (75%) had type 2 Later-Onset phenotype.Conclusions Compared with previous findings, reanalysis of 63 studies increased the screenee numbers (~3.4-fold), eliminated 20 benign/likely benign variants, and provided more accurate sex-specific and phenotype-specific prevalence estimates, ranging from ~0.13% of stroke to ~0.9% of cardiac male or female screenees.