Rare Diseases Symptoms Automatic Extraction
Home
A random Abstract
Our Project
Our Team
Autophagy-lysosome pathway associated neuropathology and axonal degeneration in the brains of alpha-galactosidase A-deficient mice.
[fabry disease]
Mutations
in
the
gene
for
alpha-galactosidase
A
result
in
Fabry
disease
,
a
rare
,
X-
linked
lysosomal
storage
disorder
characterized
by
a
loss
of
alpha-galactosidase
A
enzymatic
activity
.
The
resultant
accumulation
of
glycosphingolipids
throughout
the
body
leads
to
widespread
vasculopathy
with
particular
detriment
to
the
kidneys
,
heart
and
nervous
system
.
Disruption
in
the
autophagy-lysosome
pathway
has
been
documented
previously
in
Fabry
disease
but
its
relative
contribution
to
nervous
system
pathology
in
Fabry
disease
is
unknown
.
Using
an
experimental
mouse
model
of
Fabry
disease
,
alpha-galactosidase
A
deficiency
,
we
examined
brain
pathology
in
20
-
24
month
old
mice
with
particular
emphasis
on
the
autophagy-lysosome
pathway
.
Alpha
-galactosidase
A-
deficient
mouse
brains
exhibited
enhanced
punctate
perinuclear
immunoreactivity
for
the
autophagy
marker
microtubule-associated
protein
light-chain
3
(
LC
3
)
in
the
parenchyma
of
several
brain
regions
,
as
well
as
enhanced
parenchymal
and
vascular
immunoreactivity
for
lysosome-associated
membrane
protein-
1
(
LAMP-
1
)
.
Ultrastructural
analysis
revealed
endothelial
cell
inclusions
with
electron
densities
and
a
pronounced
accumulation
of
electron-
dense
lipopigment
.
The
pons
of
alpha-galactosidase
A-
deficient
mice
in
particular
exhibited
a
striking
neuropathological
phenotype
,
including
the
presence
of
large
,
swollen
axonal
spheroids
indicating
axonal
degeneration
,
in
addition
to
large
interstitial
aggregates
positive
for
phosphorylated
alpha-synuclein
that
co
-
localized
with
the
axonal
spheroids
.
Double
-label
immunofluorescence
revealed
co
-localization
of
phosphorylated
alpha-synuclein
aggregates
with
ubiquitin
and
LC
3
.
Together
these
findings
indicate
widespread
neuropathology
and
focused
axonal
neurodegeneration
in
alpha-galactosidase
A-
deficient
mouse
brain
in
association
with
disruption
of
the
autophagy-lysosome
pathway
,
and
provide
the
basis
for
future
mechanistic
assessment
of
the
contribution
of
the
autophagy-lysosome
pathway
to
this
histologic
phenotype
.
Diseases
Validation
Diseases presenting
"neurodegeneration"
symptom
adrenomyeloneuropathy
alexander disease
cadasil
canavan disease
classical phenylketonuria
fabry disease
gm1 gangliosidosis
hereditary cerebral hemorrhage with amyloidosis
krabbe disease
neonatal adrenoleukodystrophy
neuralgic amyotrophy
oculocutaneous albinism
pyruvate dehydrogenase deficiency
triple a syndrome
wolf-hirschhorn syndrome
x-linked adrenoleukodystrophy
zellweger syndrome
This symptom has already been validated
