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Cytochrome P450 oxidoreductase deficiency: identification and characterization of biallelic mutations and genotype-phenotype correlations in 35 Japanese patients.
[aromatase deficiency]
Cytochrome
P
450
oxidoreductase
(
POR
)
deficiency
is
a
rare
autosomal
recessive
disorder
characterized
by
skeletal
dysplasia
,
adrenal
dysfunction
,
disorders
of
sex
development
(
DSD
)
,
and
maternal
virilization
during
pregnancy
.
Although
multiple
studies
have
been
performed
for
this
condition
,
several
matters
remain
to
be
clarified
,
including
the
presence
of
manifesting
heterozygosity
and
the
underlying
factors
for
clinical
variability
.
The
objective
of
the
study
was
to
examine
such
unresolved
matters
by
detailed
molecular
studies
and
genotype-phenotype
correlations
.
Thirty
-
five
Japanese
patients
with
POR
deficiency
participated
in
the
study
.
Mutation
analysis
revealed
homozygosity
for
R
457
H
in
cases
1
-
14
(
group
A
)
,
compound
heterozygosity
for
R
457
H
and
one
apparently
null
mutation
in
cases
15
-
28
(
group
B
)
,
and
other
combinations
of
mutations
in
cases
29
-
35
(
group
C
)
.
In
particular
,
FISH
and
RT-PCR
sequencing
analyses
revealed
an
intragenic
microdeletion
in
one
apparent
R
457
H
homozygote
,
transcription
failure
of
apparently
normal
alleles
in
three
R
457
H
heterozygotes
,
and
nonsense
mediated
mRNA
decay
in
two
frameshift
mutation
-
positive
cases
examined
.
Genotype-phenotype
correlations
indicated
that
skeletal
features
were
definitely
more
severe
,
and
adrenal
dysfunction
,
46
,
XY
DSD
,
and
pubertal
failure
were
somewhat
more
severe
in
group
B
than
group
A
,
whereas
46
,
XX
DSD
and
maternal
virilization
during
pregnancy
were
similar
between
two
groups
.
Notable
findings
also
included
the
contrast
between
infrequent
occurrence
of
46
,
XY
DSD
and
invariable
occurrence
of
46
,
XX
DSD
and
pubertal
growth
pattern
in
group
A
mimicking
that
of
aromatase
deficiency
.
The
results
argue
against
the
heterozygote
manifestation
and
suggest
that
the
residual
POR
activity
reflected
by
the
R
457
H
dosage
constitutes
the
underlying
factor
for
clinical
variability
in
some
features
but
not
other
features
,
probably
due
to
the
simplicity
and
complexity
of
POR
-dependent
metabolic
pathways
relevant
to
each
phenotype
.
Diseases
Validation
Diseases presenting
"adrenal dysfunction"
symptom
adrenal incidentaloma
aromatase deficiency
congenital adrenal hyperplasia
cushing syndrome
triple a syndrome
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