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Decidual β-carotene-15,15'-oxygenase-1 and 2 (BCMO1,2) expression is increased in nitrofen model of congenital diaphragmatic hernia.
[congenital diaphragmatic hernia]
Retinoids
are
essential
for
fetal
and
lung
development
.
Beta
-carotene
(
BC
)
is
the
main
dietary
retinoid
source
and
beta
-carotene-
15
,
15
'
-
oxygenase-
1
and
2
(
Bcmo
1
,
2
)
is
the
primary
enzyme
generating
retinoid
from
BC
in
adult
mammalian
tissues
.
Placenta
has
a
major
role
in
the
retinol
homeostasis
in
fetal
life
:
Since
there
is
no
fetal
retinol
synthesis
,
maternal
retinol
has
to
cross
the
placenta
.
It
has
been
recently
shown
that
BC
can
be
converted
to
retinol
by
Bcmo
1
,
2
in
placenta
for
retinol
transfer
and
moreover
,
BC
can
cross
the
placenta
intact
.
The
placental
Bcmo
1
,
2
expression
is
tightly
controlled
by
placental
retinol
level
.
In
severe
retinol
deficiency
it
has
been
shown
that
placental
Bcmo
1
,
2
expression
are
increased
for
generating
retinol
from
dietary
maternal
BC
even
when
the
main
retinol
transfer
is
blocked
.
In
recent
years
,
low
pulmonary
retinol
levels
and
disrupted
retinoid
signaling
pathway
have
been
implicated
in
the
pathogenesis
of
pulmonary
hypoplasia
and
congenital
diaphragmatic
hernia
(
CDH
)
in
the
nitrofen
model
of
CDH
.
Recently
,
it
has
been
demonstrated
that
the
main
retinol
transfer
in
the
placenta
is
blocked
in
the
nitrofen
model
of
CDH
causing
increased
placental
and
decreased
serum
retinol
level
.
The
aim
of
our
study
was
to
determine
maternal
and
fetal
β-carotene
levels
and
to
investigate
the
hypothesis
that
placental
expression
of
BCMO
1
and
BCMO
2
is
altered
in
nitrofen-exposed
rat
fetuses
with
CDH
.
Pregnant
rats
were
exposed
to
either
olive
oil
or
nitrofen
on
day
9
of
gestation
(
D
9
)
.
Maternal
and
fetal
serum
,
placenta
,
liver
and
left
lungs
were
harvested
on
D
21
and
divided
into
two
groups
:
control
(
n
Â
=
Â
8
)
and
nitrofen
with
CDH
(
n
Â
=
Â
8
)
.
Immunochistochemistry
was
performed
to
evaluate
trophoblasts
by
cytokeratin
expression
and
placental
Bcmo
1
,
2
expression
.
Expression
levels
of
Bcmo
1
,
2
genes
in
fetal
lungs
and
liver
were
determined
using
RT-PCR
and
immunohistochemistry
.
BC
level
was
measured
using
HPLC
.
Markedly
increased
decidual
Bcmo
1
,
2
immunoreactivity
was
observed
in
CDH
group
compared
to
controls
.
There
was
no
difference
neither
in
the
trophoblastic
Bcmo
1
,
2
immunoreactivity
nor
in
the
pulmonary
and
liver
Bcmo
1
,
2
expression
compared
to
controls
.
There
was
no
significant
difference
in
maternal
serum
BC
levels
between
control
and
CDH
mothers
(
2
.
14
Â
±
Â
0
.
55
vs
2
.
56
Â
±
Â
1
.
6
Â
μM
/
g
,
p
Â
=
Â
0
.
8
)
.
BC
was
not
detectable
neither
in
the
fetal
serum
nor
liver
or
lungs
.
Our
data
show
that
nitrofen
increases
maternal
but
not
fetal
Bcmo
1
,
2
expression
in
the
placenta
Â
in
nitrofen-induced
CDH
group
.
The
markedly
increased
decidual
Bcmo
1
,
2
expression
suggests
that
nitrofen
may
trigger
local
,
decidual
retinol
synthesis
in
the
nitrofen
model
of
CDH
.
Diseases
Validation
Diseases presenting
"fetal life"
symptom
aromatase deficiency
congenital adrenal hyperplasia
congenital diaphragmatic hernia
congenital toxoplasmosis
harlequin ichthyosis
hirschsprung disease
kallmann syndrome
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