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Mutations in novel peroxin gene PEX26 that cause peroxisome-biogenesis disorders of complementation group 8 provide a genotype-phenotype correlation.
[neonatal adrenoleukodystrophy]
The
human
disorders
of
peroxisome
biogenesis
(
PBDs
)
are
subdivided
into
12
complementation
groups
(
CGs
)
.
CG
8
is
one
of
the
more
common
of
these
and
is
associated
with
varying
phenotypes
,
ranging
from
the
most
severe
,
Zellweger
syndrome
(
ZS
)
,
to
the
milder
neonatal
adrenoleukodystrophy
(
NALD
)
and
infantile
Refsum
disease
(
IRD
)
.
PEX
26
,
encoding
the
305
-
amino-acid
membrane
peroxin
,
has
been
shown
to
be
deficient
in
CG
8
.
We
studied
the
PEX
26
genotype
in
fibroblasts
of
eight
CG
8
patients--
four
with
the
ZS
phenotype
,
two
with
NALD
,
and
two
with
IRD
.
Catalase
was
mostly
cytosolic
in
all
these
cell
lines
,
but
import
of
the
proteins
that
contained
PTS
1
,
the
SKL
peroxisome
targeting
sequence
,
was
normal
.
Expression
of
PEX
26
reestablished
peroxisomes
in
all
eight
cell
lines
,
confirming
that
PEX
26
defects
are
pathogenic
in
CG
8
patients
.
When
cells
were
cultured
at
30
degrees
C
,
catalase
import
was
restored
in
the
cell
lines
from
patients
with
the
NALD
and
IRD
phenotypes
,
but
to
a
much
lesser
extent
in
those
with
the
ZS
phenotype
,
indicating
that
temperature
sensitivity
varied
inversely
with
the
severity
of
the
clinical
phenotype
.
Several
types
of
mutations
were
identified
,
including
homozygous
G
8
9
R
mutations
in
two
patients
with
ZS
.
Expression
of
these
PEX
26
mutations
in
pex
26
Chinese
hamster
ovary
cells
resulted
in
cell
phenotypes
similar
to
those
in
the
human
cell
lines
.
These
findings
confirm
that
the
degree
of
temperature
sensitivity
in
pex
26
cell
lines
is
predictive
of
the
clinical
phenotype
in
patients
with
PEX
26
deficiency
.
Diseases
Validation
Diseases presenting
"pex26 deficiency"
symptom
neonatal adrenoleukodystrophy
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