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A random Abstract
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Involvement of Werner syndrome protein in MUTYH-mediated repair of oxidative DNA damage.
[werner syndrome]
Reactive
oxygen
species
constantly
generated
as
by
-products
of
cellular
metabolism
readily
attack
genomic
DNA
creating
mutagenic
lesions
such
as
7
,
8
-
dihydro-
8
-
oxo-guanine
(
8
-
oxo-
G
)
that
promote
aging
.
8
-
oxo-
G
:
A
mispairs
arising
during
DNA
replication
are
eliminated
by
base
excision
repair
initiated
by
the
MutY
DNA
glycosylase
homologue
(
MUTYH
)
.
Here
,
by
using
formaldehyde
crosslinking
in
mammalian
cell
extracts
,
we
demonstrate
that
the
WRN
helicase
/
exonuclease
defective
in
the
premature
aging
disorder
Werner
syndrome
(
WS
)
is
recruited
to
DNA
duplex
containing
an
8
-
oxo-
G
:
A
mispair
in
a
manner
dependent
on
DNA
polymerase
λ
(
Pol
λ
)
that
catalyzes
accurate
DNA
synthesis
over
8
-
oxo-
G
.
Similarly
,
by
immunofluorescence
,
we
show
that
Pol
λ
is
required
for
accumulation
of
WRN
at
sites
of
8
-
oxo-
G
lesions
in
human
cells
.
Moreover
,
we
show
that
nuclear
focus
formation
of
WRN
and
Pol
λ
induced
by
oxidative
stress
is
dependent
on
ongoing
DNA
replication
and
on
the
presence
of
MUTYH
.
Cell
viability
assays
reveal
that
depletion
of
MUTYH
suppresses
the
hypersensitivity
of
cells
lacking
WRN
and
/
or
Pol
λ
to
oxidative
stress
.
Biochemical
studies
demonstrate
that
WRN
binds
to
the
catalytic
domain
of
Pol
λ
and
specifically
stimulates
DNA
gap
filling
by
Polλ
over
8
-
oxo-
G
followed
by
strand
displacement
synthesis
.
Our
results
suggest
that
WRN
promotes
long
-patch
DNA
repair
synthesis
by
Pol
λ
during
MUTYH
-initiated
repair
of
8
-
oxo-
G
:
A
mispairs
.
Diseases
Validation
Diseases presenting
"accumulation of wrn"
symptom
werner syndrome
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