[The switch of enzyme therapy in Fabry disease].

[fabry disease]

Fabry disease (FD ) is a multiorgan X-linked lysosomal storage disorder resulted from the deficiency of the lysosomal enzyme alpha galactosidase A . It particularly affects the heart , kidneys and cerebrovascular system . The treatment options for FD patients include long -term enzyme replacement therapy (ERT ). Two recombinant enzyme formulations for the ERT of FD are available on European market : agalsidase alfa and agalsidase beta . Numerous evidences in the literature have confirmed the safety and efficacy of ERT . However , to date , there have been limited comparisons between the two agents , and no firm conclusion can be drawn regarding their specific efficacy and safety . In June 2009 , a viral contamination in the manufacturing process of Fabrazyme led to a global shortage of agalsidase beta . Recommendations to shift patients to the recommended dose of Replagal were published by the European Medicines Agency (EMA ) for all patients receiving Fabrazyme . This offered the unique opportunity to compare , although indirectly , the two drugs evaluating any clinical modification or adverse events that occurred after the switch . Moreover , with the increased availability of agalsidase beta in the last 3 months of 2012 , some of the patients who previously switched to agalsidase alfa , were switched-back and returned to full-dose agalsidase beta . This article reviews the published evidence for the clinical efficacy of the two available enzyme preparations and compare it with the experience of our center .