Rare Diseases Symptoms Automatic Extraction
Home
A random Abstract
Our Project
Our Team
Rapamycin decreases DNA damage accumulation and enhances cell growth of WRN-deficient human fibroblasts.
[werner syndrome]
Werner
syndrome
(
WS
)
,
caused
by
mutations
at
the
WRN
helicase
gene
,
is
a
progeroid
syndrome
characterized
by
multiple
features
consistent
with
accelerated
aging
.
Aberrant
double
-strand
DNA
damage
repair
leads
to
genomic
instability
and
reduced
replicative
lifespan
of
somatic
cells
.
We
observed
increased
autophagy
in
WRN
knockdown
cells
;
this
was
further
increased
by
short
-term
rapamycin
treatment
.
Long
-term
rapamycin
treatment
resulted
in
improved
growth
rate
,
reduced
accumulation
of
DNA
damage
foci
and
improved
nuclear
morphology
;
autophagy
markers
were
reduced
to
near-normal
levels
,
possibly
due
to
clearance
of
damaged
proteins
.
These
data
suggest
that
protein
aggregation
plays
a
role
in
the
development
of
WS
phenotypes
and
that
the
mammalian
target
of
rapamycin
complex
1
pathway
is
a
potential
therapeutic
target
of
WS
.
Diseases
Validation
Diseases presenting
"growth rate"
symptom
classical phenylketonuria
dedifferentiated liposarcoma
liposarcoma
proteus syndrome
werner syndrome
You can validate or delete this automatically detected symptom
Validate the Symptom
Delete the Symptom