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[X-linked adrenoleukodystrophy].
[adrenomyeloneuropathy]
X-
linked
adrenoleukodystrophy
(
ALD
)
is
a
severe
neurodegenerative
disorder
.
ALD
is
characterized
by
progressive
demyelination
within
the
central
and
peripheral
nervous
system
,
adrenal
insufficiency
(
Addison
's
disease
)
and
accumulation
of
very
-
long
-chain
fatty
acids
(
VLCFA
)
in
plasma
,
fibroblasts
and
tissues
.
The
overall
incidence
of
ALD
is
1
:
17
,
000
including
hemizygotes
and
heterozygotes
who
are
frequently
symptomatic
.
There
are
two
main
ALD
phenotypes
:
1
)
a
cerebral
demyelinating
form
which
affects
boys
between
5
-
12
years
,
but
also
35
%
of
adult
males
;
2
)
a
form
that
mainly
involves
the
spinal
cord
(
adrenomyeloneuropathy
,
AMN
)
in
adult
males
between
20
-
50
years
and
50
%
of
heterozygous
women
after
the
age
of
40
years
.
AMN
presents
with
progressive
spastic
paraparesis
.
Addison
's
disease
may
be
the
first
symptom
of
ALD
in
boys
and
adult
males
.
These
patients
are
at
risk
to
develop
cerebral
ALD
or
AMN
for
life
.
ALD
results
from
mutations
in
the
ABCD
1
gene
without
correlation
between
genotype
and
phenotype
.
The
diagnosis
of
ALD
relies
upon
the
measurement
of
plasma
VLCFA
levels
that
allows
the
identification
of
100
%
affected
males
and
of
80
-
95
%
heterozygous
women
.
Because
of
these
false-negative
,
it
is
therefore
mandatory
to
search
for
a
mutation
in
the
ABCD
1
gene
in
all
women
at
risk
to
be
heterozygous
for
ALD
.
The
ABCD
1
gene
encodes
a
peroxisomal
transmembrane
protein
(
ALD
protein
)
with
the
structure
of
an
half
ATP-binding
cassette
transporter
.
It
is
possible
that
ALD
protein
imports
VLCFA
or
VLCFA-CoA
into
peroxisomes
in
which
they
are
degraded
by
a
peroxisomal
beta
-oxidation
system
.
Elongation
of
VLCFAs
is
enhanced
in
fibroblasts
from
ALD
patients
and
likely
contributes
to
the
load
of
VLCFA
in
tissues
.
The
underlying
mechanisms
that
lead
to
cerebral
demyelination
,
axonal
degeneration
in
spinal
cord
and
adrenal
insufficiency
are
unknown
.
The
"
toxic
"
role
of
VLCFA
accumulation
remains
to
be
demonstrated
.
The
mechanisms
that
lead
to
the
inflammatory
reaction
in
cerebral
ALD
might
involve
abnormal
acylation
of
gangliosides
and
phospholipids
by
VLCFA
that
would
result
in
immune
reaction
of
brain
macrophages
and
astrocytes
bearing
CD
1
molecules
that
recognize
lipid
antigens
.
De
novo
mutation
of
ABCD
1
occurs
in
less
than
8
%
of
ALD
patients
.
The
genetic
counseling
aims
to
identify
:
1
)
women
who
are
at
risk
to
be
heterozygous
;
2
)
neurologically
asymptomatic
boys
.
It
is
only
at
this
stage
that
allogeneic
bone
marrow
transplantation
has
clinical
benefit
;
3
)
ALD
patients
who
have
Addison
's
disease
that
can
lead
to
sudden
death
.
Prenatal
diagnosis
(
chorionic
villus
samples
,
cultured
amniotic
fluid
cells
)
relies
upon
DNA
based
mutation
detection
techniques
,
expression
of
ALD
protein
and
measurement
of
VLCFA
levels
.
Allogeneic
bone
marrow
transplantation
is
the
only
treatment
that
provides
a
permanent
cure
when
the
procedure
is
performed
at
an
early
stage
of
cerebral
demyelination
,
i
.
e
when
the
patients
are
asymptomatic
despite
abnormal
brain
MRI
.
Treatment
of
Addison
's
disease
is
mandatory
but
does
not
modify
the
course
of
neurological
symptoms
.
Dietary
therapy
failed
to
halt
the
neurologic
progression
in
cerebral
ALD
and
AMN
.
It
might
have
a
partial
preventive
effect
in
boys
treated
before
6
years
of
age
.
Diseases
Validation
Diseases presenting
"abnormal acylation"
symptom
adrenomyeloneuropathy
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