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Chemoprevention of esophageal adenocarcinoma in a rat model by ursodeoxycholic acid.
[esophageal adenocarcinoma]
Reflux
of
bile
acid
into
the
esophagus
induces
esophagitis
,
inflammation
-stimulated
hyperplasia
,
metaplasia
such
as
Barrett
's
esophagus
(
BE
)
,
and
esophageal
adenocarcinoma
(
EAC
)
.
Caudal-
type
homeobox
2
(
Cdx
2
)
via
nuclear
factor
(
NF
)
-
κB
induced
by
bile
acid
is
an
important
factor
in
the
development
of
BE
and
EAC
.
In
colorectal
cancer
,
experimental
data
suggest
a
chemopreventive
effect
of
ursodeoxycholic
acid
(
UDCA
)
.
We
hypothesized
that
UDCA
may
protect
against
the
esophageal
inflammation
-metaplasia-carcinoma
sequence
by
decreasing
the
overall
proportion
of
the
toxic
bile
acids
.
Wistar
male
rats
that
underwent
a
duodenoesophageal
reflux
procedure
were
divided
into
two
groups
.
One
group
was
given
commercial
chow
(
control
group
)
,
and
the
other
was
given
experimental
chow
containing
UDCA
(
UDCA
group
)
.
The
animals
were
killed
at
40
Â
weeks
after
surgery
,
and
their
bile
and
esophagus
were
examined
.
In
the
UDCA
group
,
the
esophagitis
was
milder
and
the
incidence
of
BE
was
significantly
lower
(
p
Â
<
Â
0
.
05
)
than
in
the
control
group
,
and
EAC
was
not
observed
(
p
Â
<
Â
0
.
05
)
.
In
analysis
of
the
compartment
of
bile
acid
,
UDCA
was
markedly
increased
in
the
UDCA
group
compared
with
the
control
group
(
32
.
7
Â
±
Â
11
.
4
vs
.
0
.
82
Â
±
Â
0
.
33
Â
mmol
/
L
,
p
Â
<
Â
0
.
05
)
and
cholic
acid
was
decreased
(
32
.
7
Â
±
Â
4
.
05
vs
.
60
.
9
Â
±
Â
8
.
26
Â
mmol
/
L
,
p
Â
<
Â
0
.
05
)
.
Expression
intensity
of
Cdx
2
and
NF-κB
was
greater
in
the
control
group
than
in
the
UDCA
group
(
p
Â
<
Â
0
.
05
)
.
UDCA
may
be
a
chemopreventive
agent
against
EAC
by
varying
the
bile
acid
composition
.
Diseases
Validation
Diseases presenting
"esophagitis"
symptom
cushing syndrome
dystrophic epidermolysis bullosa
esophageal adenocarcinoma
esophageal carcinoma
esophageal squamous cell carcinoma
triple a syndrome
This symptom has already been validated