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High-mobility group AT-hook 2: an independent marker of poor prognosis in intrahepatic cholangiocarcinoma.
[cholangiocarcinoma]
High
-mobility
group
AT-hook
2
(
HMGA
2
)
regulates
cell
growth
,
differentiation
,
apoptosis
,
and
neoplastic
transformation
.
Previous
studies
have
shown
that
malignant
tumors
expressing
HMGA
2
,
such
as
gastric
,
lung
,
and
colorectal
carcinomas
,
usually
have
a
poor
prognosis
.
HMGA
2
expression
and
its
clinical
significance
in
intrahepatic
cholangiocarcinomas
have
not
been
studied
.
We
identified
55
intrahepatic
cholangiocarcinomas
resected
at
our
institution
from
1994
to
2003
.
Hematoxylin-eosin-stained
slides
were
reviewed
,
and
histopathologic
characteristics
were
recorded
,
including
mitotic
count
,
tumor
grade
,
vascular
and
perineural
invasion
,
lymph
node
metastasis
,
and
margin
status
.
Using
immunohistochemical
stains
,
we
examined
expression
of
HMGA
2
,
p
53
,
p
16
,
Kit
,
α-fetoprotein
,
and
Ki-
67
,
and
we
analyzed
the
correlation
of
survival
with
clinicopathological
characteristics
and
immunohistochemical
findings
.
Positive
staining
for
HMGA
2
,
p
53
,
p
16
,
Kit
,
α-fetoprotein
,
and
Ki-
67
was
seen
in
18
(
33
%
)
,
37
(
69
%
)
,
26
(
47
%
)
,
21
(
38
%
)
,
2
(
4
%
)
,
and
34
(
63
%
)
tumors
,
respectively
.
HMGA
2
expression
correlated
positively
with
p
53
expression
(
P
=
.
02
;
Ï
=
0
.
32
)
and
negatively
with
p
16
expression
(
P
=
.
04
;
Ï
=
-
0
.
28
)
.
Univariate
analysis
showed
that
HMGA
2
expression
and
lymph
node
metastasis
were
associated
with
shorter
patient
survival
and
were
independent
indicators
of
poor
survival
(
P
=
.
02
and
P
=
.
03
,
respectively
)
.
Tumorigenic
effects
of
HMGA
2
in
intrahepatic
cholangiocarcinoma
may
partly
reflect
its
ability
to
negatively
regulate
expression
of
p
16
tumor
suppressors
and
to
be
associated
with
p
53
abnormalities
.
Diseases
Validation
Diseases presenting
"intrahepatic cholangiocarcinoma"
symptom
carcinoma of the gallbladder
cholangiocarcinoma
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