De novo mutation in a male patient with Fabry disease: a case report.

[fabry disease]

Fabry disease is an X-linked inherited metabolic condition where the deficit of the α-galactosidase A enzyme , encoded by the GLA gene , leads to glycosphingolipid storage , mainly globotriaosylceramide . To date , more than 600 mutations have been identified in human GLA gene that are responsible for FD , including missense and nonsense mutations , small and large deletions . Such mutations are usually inherited , and cases of de novo onset occur rarely .In this article we report an interesting case of a 44 -year -old male patient suffering from a severe form of Fabry disease , with negative family history . The patient showed signs such as cornea verticillata , angiokeratomas , cardiac and neurological manifestations , an end-stage renal disease and he had low α-galactosidase A activity . We detected , in this subject , the mutation c .493 G > C in the third exon of the GLA gene which causes the amino acid substitution D 165 H in the protein . This mutation affects the amino acid - belonging to the group of buried residues - involved , probably , in the preservation of the protein folding . Moreover , studies of multiple sequence alignment indicate that this amino acid is highly conserved , thus strengthening the hypothesis that it is a key amino acid to the enzyme functionality .The study of the relatives of the patient showed that , surprisingly , none of the members of his family of origin had this genetic alteration , suggesting a de novo mutation . Only his 11 -year -old daughter - showing acroparaesthesias and heat intolerance with reduced enzymatic activity - had the same mutation .We suggest that a non-inherited mutation of the α-galactosidase A gene is responsible for Fabry disease in the patient who had reduced enzyme activity and classical clinical manifestations of the disease . In a family , it is rare to find only one Fabry disease affected subject with a de novo mutation . These findings emphasize the importance of early diagnosis , genetic counselling , studying the genealogical tree of the patients and starting enzyme replacement therapy to prevent irreversible vital organ damage that occurs during the course of the disease .