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Identification of a common PEX1 mutation in Zellweger syndrome.
[neonatal adrenoleukodystrophy]
The
Zellweger
spectrum
of
disease
,
encompassing
Zellweger
syndrome
and
the
progressively
milder
phenotypes
of
neonatal
adrenoleukodystrophy
and
infantile
Refsum
disease
,
is
due
to
a
failure
to
form
functional
peroxisomes
.
Cell
fusion
complementation
studies
demonstrated
that
these
diseases
are
genetically
heterogeneous
,
with
two
-thirds
of
all
patients
lying
within
a
single
complementation
group
,
CG
1
.
Molecular
genetic
and
cell
biology
studies
have
shown
that
PEX
1
is
deficient
in
many
CG
1
patients
.
However
,
previous
studies
have
focused
on
mildly
affected
patients
and
there
is
still
no
report
of
two
mutant
PEX
1
alleles
in
any
Zellweger
syndrome
patient
.
Furthermore
,
mutations
in
the
PMP
70
gene
have
also
been
identified
in
two
Zellweger
syndrome
patients
from
CG
1
,
raising
the
possibility
that
CG
1
patients
may
represent
a
mixture
of
PEX
1
-
deficient
and
PMP
70
-
deficient
individuals
.
To
address
the
molecular
basis
of
disease
in
Zellweger
syndrome
patients
from
CG
1
,
we
examined
all
24
PEX
1
exons
in
four
patients
,
including
both
patients
that
have
mutations
in
PMP
70
.
PEX
1
mutations
were
detected
in
all
four
patients
,
including
a
1
-
bp
insertion
(
c
.
2097
insT
)
in
exon
13
that
was
present
in
three
of
the
four
patients
.
Subsequent
studies
demonstrated
that
this
mutation
is
present
in
one
-
half
of
all
CG
1
patients
and
correlates
with
the
Zellweger
syndrome
phenotype
.
As
this
mutation
leads
to
a
loss
of
protein
function
its
frequency
makes
it
the
most
common
cause
of
Zellweger
syndrome
,
helping
to
explain
the
high
percentage
of
patients
that
belong
to
CG
1
.
Diseases
Validation
Diseases presenting
"deficient individuals"
symptom
homocystinuria without methylmalonic aciduria
neonatal adrenoleukodystrophy
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