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Telomerase protects werner syndrome lineage-specific stem cells from premature aging.
[werner syndrome]
Werner
syndrome
(
WS
)
patients
exhibit
premature
aging
predominantly
in
mesenchyme-derived
tissues
,
but
not
in
neural
lineages
,
a
consequence
of
telomere
dysfunction
and
accelerated
senescence
.
The
cause
of
this
lineage-
specific
aging
remains
unknown
.
Here
,
we
document
that
reprogramming
of
WS
fibroblasts
to
pluripotency
elongated
telomere
length
and
prevented
telomere
dysfunction
.
To
obtain
mechanistic
insight
into
the
origin
of
tissue-
specific
aging
,
we
differentiated
iPSCs
to
mesenchymal
stem
cells
(
MSCs
)
and
neural
stem
/
progenitor
cells
(
NPCs
)
.
We
observed
recurrence
of
premature
senescence
associated
with
accelerated
telomere
attrition
and
defective
synthesis
of
the
lagging
strand
telomeres
in
MSCs
,
but
not
in
NPCs
.
We
postulate
this
"
aging
"
discrepancy
is
regulated
by
telomerase
.
Expression
of
hTERT
or
p
53
knockdown
ameliorated
the
accelerated
aging
phenotypein
MSC
,
whereas
inhibition
of
telomerase
sensitized
NPCs
to
DNA
damage
.
Our
findings
unveil
a
role
for
telomerase
in
the
protection
of
accelerated
aging
in
a
specific
lineage
of
stem
cells
.
Diseases
Validation
Diseases presenting
"we differentiated ipscs to mesenchymal stem cells"
symptom
werner syndrome
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