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Fabry nephropathy: a review - how can we optimize the management of Fabry nephropathy?
[fabry disease]
Fabry
disease
is
a
rare
,
X-
linked
,
lysosomal
storage
disease
caused
by
mutations
in
the
gene
encoding
the
enzyme
alpha-galactosidase
A
.
Complete
or
partial
deficiency
in
this
enzyme
leads
to
intracellular
accumulation
of
globotriaosylceramide
(
Gb
3
)
and
related
glycosphingolipids
in
many
cell
types
throughout
the
body
,
including
the
kidney
.
Progressive
accumulation
of
Gb
3
in
podocytes
,
epithelial
cells
and
the
tubular
cells
of
the
distal
tubule
and
loop
of
Henle
contribute
to
the
renal
symptoms
of
Fabry
disease
,
which
manifest
as
proteinuria
and
reduced
glomerular
filtration
rate
leading
to
chronic
kidney
disease
and
progression
to
end-
stage
renal
disease
.
Early
diagnosis
and
timely
initiation
of
treatment
of
Fabry
renal
disease
is
an
important
facet
of
disease
management
.
Initiating
treatment
with
enzyme
replacement
therapy
(
ERT
;
agalsidase
alfa
,
Replagal
®
,
Shire
;
agalsidase
beta
,
Fabrazyme
®
,
Genzyme
)
as
part
of
a
comprehensive
strategy
to
prevent
complications
of
the
disease
,
may
be
beneficial
in
stabilizing
renal
function
or
slowing
its
decline
.
Early
initiation
of
ERT
may
also
be
more
effective
than
initiating
therapy
in
patients
with
more
advanced
disease
.
Several
strategies
are
required
to
complement
the
use
of
ERT
and
treat
the
myriad
of
associated
symptoms
and
organ
involvements
.
In
particular
,
patients
with
renal
Fabry
disease
are
at
risk
of
cardiovascular
events
,
such
as
high
blood
pressure
,
cardiac
arrhythmias
and
stroke
.
This
review
discusses
the
management
of
renal
involvement
in
Fabry
disease
,
including
diagnosis
,
treatments
,
and
follow-up
,
and
explores
recent
advances
in
the
use
of
biomarkers
to
assist
with
diagnosis
,
monitoring
disease
progression
and
response
to
treatment
.
Diseases
Validation
Diseases presenting
"early diagnosis"
symptom
achondroplasia
acute rheumatic fever
adrenal incidentaloma
adrenomyeloneuropathy
alexander disease
allergic bronchopulmonary aspergillosis
aromatase deficiency
carcinoma of the gallbladder
cholangiocarcinoma
classical phenylketonuria
coats disease
cohen syndrome
congenital adrenal hyperplasia
congenital diaphragmatic hernia
congenital toxoplasmosis
cowden syndrome
cushing syndrome
cutaneous mastocytosis
cystinuria
dentin dysplasia
dentinogenesis imperfecta
dracunculiasis
erdheim-chester disease
erythropoietic protoporphyria
esophageal carcinoma
esophageal squamous cell carcinoma
fabry disease
familial hypocalciuric hypercalcemia
familial mediterranean fever
gm1 gangliosidosis
hirschsprung disease
holt-oram syndrome
homocystinuria without methylmalonic aciduria
hydrocephalus with stenosis of the aqueduct of sylvius
inclusion body myositis
kabuki syndrome
kallmann syndrome
kindler syndrome
krabbe disease
locked-in syndrome
monosomy 21
neuralgic amyotrophy
oculocutaneous albinism
oligodontia
omenn syndrome
oral submucous fibrosis
papillon-lefèvre syndrome
phenylketonuria
primary effusion lymphoma
primary hyperoxaluria type 1
proteus syndrome
pyomyositis
pyruvate dehydrogenase deficiency
scrub typhus
severe combined immunodeficiency
sneddon syndrome
systemic capillary leak syndrome
thoracic outlet syndrome
triple a syndrome
typhoid
von hippel-lindau disease
wiskott-aldrich syndrome
wolf-hirschhorn syndrome
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