Fabry Disease Clinical Trial
Official title:
Improving the Diagnostic Rate of Fabry Disease in Patients With Cerebrovascular Involvement in Taiwan- a Cohort Screening Program
Fabry disease is an X-linked disorder of glycosphingolipid catabolism caused by a deficiency
of the enzyme α-galactosidase A (α-Gal A), which leads to a progressive accumulation of
globotriaosylceramide (Gb-3) in plasma and tissue lysosomes throughout the body. Lysosomal
accumulation can result in lysosomal and cellular dysfunction, which leads to renal,
cardiac, and central nervous system (CNS) complications.
It is estimated that 1 in 40,000 males has Fabry disease, whereas the estimated prevalence
in the general population is 1 in 117,000 people. Newborn screenings for both classical and
atypical Fabry disease in Taiwan also revealed a markedly high incidence of 1 in 2,300 and 1
in 3,000 newborns. Cerebrovascular variant Fabry disease may affect up to 4.9% of male
patients and 2.4% of female patients with idiopathic stroke.
The diagnosis of Fabry disease can be challenging due to the diverse signs and symptoms,
different ages of onset, and variable timing and severity of progression. The importance of
Fabry disease lies in the irreversible renal, cardiac, cerebrovascular, and neurological
damage. An early diagnosis of Fabry disease is important for initiating symptom management
and reducing life-threatening complications, as well as for early identification of other
affected family members. Therefore, the present study would like to conduct further
screening of high-risk group of early cerebrovascular involvement that is essential for the
successful management of Fabry disease.
This is a cross-sectional, population-based study to identify Fabry disease in patients with
early cerebrovascular involvement. Eligible patients are age above 18 years old (<=55 years
old) with early cerebrovascular involvement and have provided inform consent. Patients who
have been diagnosed Fabry disease are not eligible.
The present study will use samples of early cerebrovascular involvement patients which have
been enrolled in two previous IRB approved projects [103-3254C (origin 98-3889A3), 100-4008C
(origin 97-0470B)], participants of both studies have consented that participants' samples
could be further investigated if needed.
Since, the investigators cannot ensure whether the condition of enzyme activity of frozen
plasma sample were decayed after long-term storage and the investigators don't have
available normal range of enzyme activity of historical plasma sample, the investigators
will perform specific genotyping of Fabry disease for these patients according to the
specific mutation variants which have been identified in Taiwan population previously.
Patients will be recalled to assess Fabry related symptoms if genetic testing has mutation
finding and family screening will be performed if applicable. Further inform consent will be
obtained as well.
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Observational Model: Cohort, Time Perspective: Retrospective
| Status | Clinical Trial | Phase | |
|---|---|---|---|
| Recruiting |
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