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Evaluation of prenatal intra-amniotic LAMB3 gene delivery in a mouse model of Herlitz disease.
[junctional epidermolysis bullosa]
Prenatal
gene
therapy
has
been
considered
for
Herlitz
junctional
epidermolysis
bullosa
(
H-
JEB
)
,
a
lethal
genodermatosis
caused
by
the
absence
of
any
of
the
three
subunits
of
laminin-
5
,
resulting
from
birth
in
widespread
blistering
and
erosions
of
skin
and
mucosae
.
To
investigate
this
strategy
in
an
animal
model
,
adenovirus
type
5
-
and
adeno-associated
virus
(
AAV
)
type
2
-
derived
vectors
carrying
a
beta
-galactosidase
reporter
gene
or
LAMB
3
cDNA
encoding
the
beta
3
chain
of
laminin-
5
were
generated
,
tested
for
stability
in
amniotic
fluid
and
evaluated
in
vitro
on
murine
H-
JEB
keratinocytes
,
and
in
vivo
by
prenatal
injection
into
the
amniotic
cavities
of
laminin-
5
beta
3
-
deficient
mice
.
The
different
vectors
were
administered
individually
or
combined
at
maximum
doses
on
day
14
post
coitum
.
Adenoviral
vectors
infected
preferentially
the
foetal
epidermis
,
whereas
AAV
delivered
the
transgene
mainly
to
mucous
membranes
of
the
airways
and
the
upper
digestive
tract
.
The
LAMB
3
transgene
was
expressed
in
target
epithelia
of
newborn
laminin-
5
beta
3
-
deficient
mice
,
and
the
transgenic
beta
3
chain
was
shown
to
assemble
with
its
endogenous
partner
chains
,
resulting
in
detectable
amounts
of
laminin-
5
in
the
basement
membranes
of
skin
and
mucosae
and
in
a
lower
extent
of
tissue
separation
in
the
skin
.
However
,
only
combined
delivery
of
the
two
vector
types
led
to
a
minor
increase
of
the
life
span
of
H-
JEB
mice
.
Failure
to
rescue
diseased
animals
was
,
at
least
in
part
,
due
to
abandonment
of
any
conspicuous
pup
by
the
heterozygous
mother
.
This
is
the
first
study
of
a
prenatal
gene
therapy
approach
to
a
heritable
blistering
disorder
.
Although
our
findings
indicate
that
prenatal
combined
administration
of
adenoviral
and
adeno-associated
LAMB
3
vectors
provides
therapeutic
benefit
to
H-
JEB
mice
,
this
animal
model
appears
unsuitable
for
long
-term
investigations
of
the
therapeutic
concept
.
Diseases
Validation
Diseases presenting
"and the transgenic beta3 chain was shown to assemble with its endogenous partner chains"
symptom
junctional epidermolysis bullosa
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