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Pendrin function and regulation in Xenopus oocytes.
[pendred syndrome]
SLC
26
A
4
/
PDS
mutations
cause
Pendred
Syndrome
and
non-syndromic
deafness
.
but
some
aspects
of
function
and
regulation
of
the
SLC
26
A
4
polypeptide
gene
product
,
pendrin
,
remain
controversial
or
incompletely
understood
.
We
have
therefore
extended
the
functional
analysis
of
wildtype
and
mutant
pendrin
in
Xenopus
oocytes
,
with
studies
of
isotopic
flux
,
electrophysiology
,
and
protein
localization
.
Pendrin
mediated
electroneutral
,
pH-insensitive
,
DIDS-insensitive
anion
exchange
,
with
extracellular
K
(
(
1
/
2
)
)
(
in
mM
)
of
1
.
9
(
Cl
(
-
)
)
,
1
.
8
(
I
(
-
)
)
,
and
0
.
9
(
Br
(
-
)
)
.
The
unusual
phenotype
of
Pendred
Syndrome
mutation
E
303
Q
(
loss
-of-function
with
normal
surface
expression
)
prompted
systematic
mutagenesis
at
position
303
.
Only
mutant
E
303
K
exhibited
loss
-of-function
unrescued
by
forced
overexpression
.
Mutant
E
303
C
was
insensitive
to
charge
modification
by
methanethiosulfonates
.
The
corresponding
mutants
SLC
26
A
2
E
336
Q
,
SLC
26
A
3
E
293
Q
,
and
SLC
26
A
6
E
298
Q
exhibited
similar
loss
-of-function
phenotypes
,
with
wildtype
surface
expression
also
documented
for
SLC
26
A
2
E
336
Q
.
The
strong
inhibition
of
wildtype
SLC
26
A
2
,
SLC
26
A
3
,
and
SLC
26
A
6
by
phorbol
ester
contrasts
with
its
modest
inhibition
of
pendrin
.
Phorbol
ester
inhibition
of
SLC
26
A
2
,
SLC
26
A
3
,
and
SLC
26
A
6
was
blocked
by
coexpressed
kinase-dead
PKC
δ
but
was
without
effect
on
pendrin
.
Mutation
of
SLC
26
A
2
serine
residues
conserved
in
PKC
δ
-
sensitive
SLC
26
proteins
but
absent
from
pendrin
failed
to
reduce
PKC
δ
sensitivity
of
SLC
26
A
2
(
190
)
.
Diseases
Validation
Diseases presenting
"similar loss-of-function phenotypes"
symptom
pendred syndrome
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