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Properties of astrocytes cultured from GFAP over-expressing and GFAP mutant mice.
[alexander disease]
Alexander
disease
is
a
fatal
leukoencephalopathy
caused
by
dominantly-acting
coding
mutations
in
GFAP
.
Previous
work
has
also
implicated
elevations
in
absolute
levels
of
GFAP
as
central
to
the
pathogenesis
of
the
disease
.
However
,
identification
of
the
critical
astrocyte
functions
that
are
compromised
by
mis-expression
of
GFAP
has
not
yet
been
possible
.
To
provide
new
tools
for
investigating
the
nature
of
astrocyte
dysfunction
in
Alexander
disease
,
we
have
established
primary
astrocyte
cultures
from
two
mouse
models
of
Alexander
disease
,
a
transgenic
that
over-expresses
wild
type
human
GFAP
,
and
a
knock-
in
at
the
endogenous
mouse
locus
that
mimics
a
common
Alexander
disease
mutation
.
We
find
that
mutant
GFAP
,
as
well
as
excess
wild
type
GFAP
,
promotes
formation
of
cytoplasmic
inclusions
,
disrupts
the
cytoskeleton
,
decreases
cell
proliferation
,
increases
cell
death
,
reduces
proteasomal
function
,
and
compromises
astrocyte
resistance
to
stress
.
Diseases
Validation
Diseases presenting
"excess wild type"
symptom
alexander disease
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