Fabry disease in patients under dialysis: A screening study and identification of a novel mutation
ABSTRACT Fabry disease (FD) is a rare systemic disease, with a large spectrum of disease severity. A GLA gene mutation in X‑chromosome leads to progressive accumulation of globotriaosylceramide (Gb3) in various organs. We screened all patients under dialysis from a single center for GLA gene changes. Enzymatic activity of alpha galactosidase A (α‑Gal A) and concentration of lyso‑Gb3 were determined in dried blood spots. Genetic study was performed in male patients with low α‑Gal A activity and in all female subjects. For all positive patients, a complete family study was performed. A total of 72 dialysis patients were screened. Sequence analysis was carried out in 53 patients (25 males). Heterozygous variants of the GLA gene were found in 4 patients (7.5%): c.937G>T (D313Y) in exon 6; c.352C>T (R118C) in exon 2; c.870G>C (M290I) in exon 6 and c.580A>G (T194A) in exon 4. Family screening was performed in a total of 17 subjects, with a GLA genetic variant prevalence of 58.8%. Unlike p.D313Y and p.R118C, well‑known non‑pathogenic polymorphisms, p.M290I is a controversial poorly described mutation. Reports about its phenotypic expression are crucial for a better understanding of its behavior. The recognition of the novel mutation p.T194A is importante for better knowledge of FD and its spectrum of clinical manifestations. These affected patients are expected to develop a classic and life‑threatening FD phenotype and an early diagnosis is essential for their treatment success.
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Sociedade Portuguesa de Nefrologia
2021
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oai:scielo:S0872-016920210001000292021-08-03Fabry disease in patients under dialysis: A screening study and identification of a novel mutationSilva,Francisca Gomes daPestana,NicoleDurães,JoséRosa,Nuno GuimarãesSilva,Gil Genetic Screening X‑Linked Genetic Diseases Chronic Renal Failure End‑Stage Kidney Disease Hereditary Ventricular Hypertrophy ABSTRACT Fabry disease (FD) is a rare systemic disease, with a large spectrum of disease severity. A GLA gene mutation in X‑chromosome leads to progressive accumulation of globotriaosylceramide (Gb3) in various organs. We screened all patients under dialysis from a single center for GLA gene changes. Enzymatic activity of alpha galactosidase A (α‑Gal A) and concentration of lyso‑Gb3 were determined in dried blood spots. Genetic study was performed in male patients with low α‑Gal A activity and in all female subjects. For all positive patients, a complete family study was performed. A total of 72 dialysis patients were screened. Sequence analysis was carried out in 53 patients (25 males). Heterozygous variants of the GLA gene were found in 4 patients (7.5%): c.937G>T (D313Y) in exon 6; c.352C>T (R118C) in exon 2; c.870G>C (M290I) in exon 6 and c.580A>G (T194A) in exon 4. Family screening was performed in a total of 17 subjects, with a GLA genetic variant prevalence of 58.8%. Unlike p.D313Y and p.R118C, well‑known non‑pathogenic polymorphisms, p.M290I is a controversial poorly described mutation. Reports about its phenotypic expression are crucial for a better understanding of its behavior. The recognition of the novel mutation p.T194A is importante for better knowledge of FD and its spectrum of clinical manifestations. These affected patients are expected to develop a classic and life‑threatening FD phenotype and an early diagnosis is essential for their treatment success.info:eu-repo/semantics/openAccessSociedade Portuguesa de NefrologiaPortuguese Journal of Nephrology & Hypertension v.35 n.1 20212021-03-01info:eu-repo/semantics/articletext/htmlhttp://scielo.pt/scielo.php?script=sci_arttext&pid=S0872-01692021000100029pt10.32932/pjnh.2021.04.114 |
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| author |
Silva,Francisca Gomes da Pestana,Nicole Durães,José Rosa,Nuno Guimarães Silva,Gil |
| spellingShingle |
Silva,Francisca Gomes da Pestana,Nicole Durães,José Rosa,Nuno Guimarães Silva,Gil Fabry disease in patients under dialysis: A screening study and identification of a novel mutation |
| author_facet |
Silva,Francisca Gomes da Pestana,Nicole Durães,José Rosa,Nuno Guimarães Silva,Gil |
| author_sort |
Silva,Francisca Gomes da |
| title |
Fabry disease in patients under dialysis: A screening study and identification of a novel mutation |
| title_short |
Fabry disease in patients under dialysis: A screening study and identification of a novel mutation |
| title_full |
Fabry disease in patients under dialysis: A screening study and identification of a novel mutation |
| title_fullStr |
Fabry disease in patients under dialysis: A screening study and identification of a novel mutation |
| title_full_unstemmed |
Fabry disease in patients under dialysis: A screening study and identification of a novel mutation |
| title_sort |
fabry disease in patients under dialysis: a screening study and identification of a novel mutation |
| description |
ABSTRACT Fabry disease (FD) is a rare systemic disease, with a large spectrum of disease severity. A GLA gene mutation in X‑chromosome leads to progressive accumulation of globotriaosylceramide (Gb3) in various organs. We screened all patients under dialysis from a single center for GLA gene changes. Enzymatic activity of alpha galactosidase A (α‑Gal A) and concentration of lyso‑Gb3 were determined in dried blood spots. Genetic study was performed in male patients with low α‑Gal A activity and in all female subjects. For all positive patients, a complete family study was performed. A total of 72 dialysis patients were screened. Sequence analysis was carried out in 53 patients (25 males). Heterozygous variants of the GLA gene were found in 4 patients (7.5%): c.937G>T (D313Y) in exon 6; c.352C>T (R118C) in exon 2; c.870G>C (M290I) in exon 6 and c.580A>G (T194A) in exon 4. Family screening was performed in a total of 17 subjects, with a GLA genetic variant prevalence of 58.8%. Unlike p.D313Y and p.R118C, well‑known non‑pathogenic polymorphisms, p.M290I is a controversial poorly described mutation. Reports about its phenotypic expression are crucial for a better understanding of its behavior. The recognition of the novel mutation p.T194A is importante for better knowledge of FD and its spectrum of clinical manifestations. These affected patients are expected to develop a classic and life‑threatening FD phenotype and an early diagnosis is essential for their treatment success. |
| publisher |
Sociedade Portuguesa de Nefrologia |
| publishDate |
2021 |
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http://scielo.pt/scielo.php?script=sci_arttext&pid=S0872-01692021000100029 |
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