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Chemical chaperones protect epidermolysis bullosa simplex keratinocytes from heat stress-induced keratin aggregation: involvement of heat shock proteins and MAP kinases.
[epidermolysis bullosa simplex]
Epidermolysis
bullosa
simplex
(
EBS
)
is
a
blistering
skin
disease
caused
by
mutations
in
keratin
genes
(
KRT
5
or
KRT
14
)
,
with
no
existing
therapies
.
Aggregates
of
misfolded
mutant
keratins
are
seen
in
cultured
keratinocytes
from
severe
EBS
patients
.
In
other
protein-folding
disorders
,
involvement
of
molecular
chaperones
and
the
ubiquitin-proteasome
system
may
modify
disease
severity
.
In
this
study
,
the
effects
of
heat
stress
on
keratin
aggregation
in
immortalized
cells
from
two
patients
with
EBS
(
KRT
5
)
and
a
healthy
control
were
examined
with
and
without
addition
of
various
test
compounds
.
Heat-induced
(
43
 
°
C
,
30
 
minutes
)
aggregates
were
observed
in
all
cell
lines
,
the
amount
of
which
correlated
with
the
donor
phenotype
.
In
EBS
cells
pre-exposed
to
proteasome
inhibitor
,
MG
132
,
and
p
38
-
mitogen-activated
protein
kinase
(
MAPK
)
inhibitor
,
SB
203580
,
the
proportion
of
aggregate-
positive
cells
increased
,
suggesting
a
role
of
proteasomes
and
phosphorylation
in
removing
mutated
keratin
.
In
contrast
,
aggregates
were
reduced
by
pretreatment
with
two
chemical
chaperones
,
trimethylamine
N-
oxide
(
TMAO
)
and
4
-
phenylbutyrate
(
4
-
PBA
)
.
TMAO
also
modulated
stress-induced
p
38
/
c-jun
N-
terminal
kinase
(
JNK
)
activation
and
expression
of
heat
shock
protein
(
HSPA
1
A
)
,
the
latter
of
which
colocalized
with
phosphorylated
keratin
5
in
EBS
cells
.
Taken
together
,
our
findings
suggest
therapeutic
targets
for
EBS
and
other
keratinopathies
.
Diseases
Validation
Diseases presenting
"mutations in keratin genes"
symptom
epidermolysis bullosa simplex
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