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Subgroups of enlarged vestibular aqueduct in relation to SLC26A4 mutations and hearing loss.
[pendred syndrome]
To
investigate
possible
association
of
hearing
loss
and
SLC
26
A
4
mutations
with
the
subgroups
of
enlarged
vestibular
aqueduct
(
EVA
)
morphology
in
Japanese
subjects
with
hearing
loss
.
Retrospective
multicenter
study
.
Forty
-
seven
subjects
who
had
vestibular
aqueduct
with
midpoint
diameter
>
1
mm
by
computed
tomography
of
the
temporal
bone
were
enrolled
at
multiple
sites
across
Japan
,
and
DNA
samples
and
clinical
data
were
collected
.
EVA
morphology
was
classified
into
four
subgroups
by
the
pattern
of
enlargement
:
aperture
,
aperture
and
midpoint
,
midpoint
,
and
borderline
enlargement
.
Venous
blood
DNA
samples
were
subjected
to
polymerase
chain
reaction-based
direct
sequencing
of
all
exons
and
exon-intron
boundaries
of
the
SLC
26
A
4
.
Four
novel
SLC
26
A
4
mutations
were
identified
in
the
present
study
.
SLC
26
A
4
mutations
were
detected
in
almost
all
subjects
with
aperture
,
aperture
and
midpoint
,
and
midpoint
enlargement
.
In
contrast
,
71
%
of
subjects
with
borderline
enlargement
had
no
SLC
26
A
4
mutation
.
No
significant
difference
was
found
in
the
distribution
of
truncating
and
nontruncating
SLC
26
A
4
mutations
between
the
EVA
subgroups
.
In
addition
,
no
significant
correlation
was
observed
between
the
EVA
subgroups
and
hearing
levels
,
incidence
of
hearing
fluctuation
,
or
progression
of
hearing
loss
.
Subgroups
of
EVA
morphology
were
significantly
correlated
with
the
presence
or
absence
of
SLC
26
A
4
mutation
.
In
a
subgroup
analysis
of
subjects
with
SLC
26
A
4
mutations
,
however
,
differences
in
the
EVA
subgroups
were
not
correlated
with
SLC
26
A
4
genotypes
or
characteristics
of
hearing
loss
.
NA
.
Diseases
Validation
Diseases presenting
"temporal bone"
symptom
achondroplasia
congenital toxoplasmosis
kallmann syndrome
pendred syndrome
von hippel-lindau disease
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