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Liver aging and pseudocapillarization in a Werner syndrome mouse model.
[werner syndrome]
Werner
syndrome
is
a
progeric
syndrome
characterized
by
premature
atherosclerosis
,
diabetes
,
cancer
,
and
death
in
humans
.
The
knockout
mouse
model
created
by
deletion
of
the
RecQ
helicase
domain
of
the
mouse
Wrn
homologue
gene
(
Wrn
(
∆
hel
/
∆
hel
)
)
is
of
great
interest
because
it
develops
atherosclerosis
and
hypertriglyceridemia
,
conditions
associated
with
aging
liver
and
sinusoidal
changes
.
Here
,
we
show
that
Wrn
(
∆
hel
/
∆
hel
)
mice
exhibit
increased
extracellular
matrix
,
defenestration
,
decreased
fenestration
diameter
,
and
changes
in
markers
of
liver
sinusoidal
endothelial
cell
inflammation
,
consistent
with
age-related
pseudocapilliarization
.
In
addition
,
hepatocytes
are
larger
,
have
increased
lipofuscin
deposition
,
more
frequent
nuclear
morphological
anomalies
,
decreased
mitochondria
number
,
and
increased
mitochondrial
diameter
compared
to
wild-
type
mice
.
The
Wrn
(
∆
hel
/
∆
hel
)
mice
also
have
altered
mitochondrial
function
and
altered
nuclei
.
Microarray
data
revealed
that
the
Wrn
(
∆
hel
/
∆
hel
)
genotype
does
not
affect
the
expression
of
many
genes
within
the
isolated
hepatocytes
or
liver
sinusoidal
endothelial
cells
.
This
study
reveals
that
Wrn
(
∆
hel
/
∆
hel
)
mice
have
accelerated
typical
age-related
liver
changes
including
pseudocapillarization
.
This
confirms
that
pseudocapillarization
of
the
liver
sinusoid
is
a
consistent
feature
of
various
aging
models
.
Moreover
,
it
implies
that
DNA
repair
may
be
implicated
in
normal
aging
changes
in
the
liver
.
Diseases
Validation
Diseases presenting
"liver sinusoidal endothelial cell inflammation"
symptom
werner syndrome
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