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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
"single nucleotide polymorphisms"
symptom
adrenomyeloneuropathy
alpha-thalassemia
benign recurrent intrahepatic cholestasis
congenital adrenal hyperplasia
dentin dysplasia
esophageal adenocarcinoma
esophageal carcinoma
esophageal squamous cell carcinoma
familial hypocalciuric hypercalcemia
hirschsprung disease
neonatal adrenoleukodystrophy
oculocutaneous albinism
oligodontia
pendred syndrome
primary effusion lymphoma
scrub typhus
triple a syndrome
waldenström macroglobulinemia
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