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Segregation of a new mutation in SLC26A4 and p.E47X mutation in GJB2 within a consanguineous Tunisian family affected with Pendred syndrome.
[pendred syndrome]
Recessive
mutations
of
the
SLC
26
A
4
(
PDS
)
gene
on
chromosome
7
q
31
can
cause
sensorineural
hearing
loss
with
goiter
(
Pendred
syndrome
)
or
non-syndromic
autosomal
recessive
hearing
loss
(
DFNB
4
)
.
Furthermore
,
mutations
in
the
GJB
2
gene
results
in
autosomal
recessive
(
DFNB
1
)
and
dominant
(
DFNA
3
)
non-syndromic
hearing
loss
.
The
aim
of
the
present
study
was
to
characterize
a
family
with
Pendred
syndrome
affected
by
severe
to
profound
HL
and
presenting
goiter
.
Affected
members
underwent
detailed
audiologic
examination
and
characterization
.
DNA
samples
from
family
members
were
genotyped
with
polymorphic
microsatellite
markers
and
sequencing
of
the
SLC
26
A
4
and
GJB
2
genes
was
performed
.
A
total
of
25
families
with
non-syndromic
hearing
loss
were
screened
for
the
common
p
.
E
47
X
mutation
in
the
GJB
2
gene
by
direct
dideoxy
sequencing
.
Genetic
microsatellite
analysis
showed
linkage
to
the
7
q
22
-
q
31
chromosomal
region
and
mutation
analysis
revealed
a
novel
frameshift
mutation
(
c
.
451
delG
)
in
the
SLC
26
A
4
gene
.
Screening
of
the
GJB
2
gene
in
one
patient
,
displayed
a
homozygous
p
.
E
47
X
mutation
,
together
with
a
heterozygous
c
.
451
delG
mutation
.
Screening
of
25
families
with
HL
showed
frequent
segregation
of
the
p
.
E
47
X
mutation
,
which
was
homozygous
in
five
of
these
families
.
Haplotype
analysis
using
microsatellite
markers
and
single
nucleotide
polymorphisms
(
SNPs
)
closely
flanking
the
GJB
2
gene
,
revealed
the
presence
of
two
disease-associated-haplotypes
suggesting
the
presence
of
at
least
,
two
founder
effects
carrying
the
p
.
E
47
X
non-sense
mutation
in
the
Tunisian
population
.
T
he
segregation
of
both
SLC
26
A
4
and
GJB
2
mutations
in
the
family
illustrates
once
again
the
unexpected
intra-familial
genetic
heterogeneity
in
consanguineous
families
and
highlights
the
difficulty
of
genetic
counselling
in
such
families
.
In
addition
,
our
results
disclose
the
existence
of
founder
effects
in
the
Tunisian
population
.
Diseases
Validation
Diseases presenting
"characterization"
symptom
pendred syndrome
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