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Association of promoter methylation of RUNX3 gene with the development of esophageal cancer: a meta analysis.
[esophageal adenocarcinoma]
Runt-related
transcription
factor
3
(
RUNX
3
)
is
a
member
of
the
runt-domain
family
of
transcription
factors
.
Emerging
evidence
indicates
that
RUNX
3
is
a
tumor
suppressor
gene
in
several
types
of
human
cancers
including
esophageal
cancer
.
However
,
the
association
between
RUNX
3
promoter
methylation
and
esophageal
cancer
remains
unclear
.
Here
we
conducted
a
systematic
review
and
meta
-analysis
to
quantitatively
evaluate
the
effects
of
RUNX
3
promoter
methylation
on
the
incidence
of
esophageal
cancer
.
A
detailed
literature
search
was
made
on
Medline
,
Pubmed
and
Web
of
Science
for
related
research
publications
written
in
English
and
/
or
Chinese
.
Methodological
quality
of
the
studies
was
also
evaluated
.
The
data
were
extracted
and
assessed
by
two
reviewers
independently
.
Analysis
of
pooled
data
were
performed
,
the
odds
ratios
(
OR
)
were
calculated
and
summarized
respectively
.
Final
analysis
of
558
patients
from
9
eligible
studies
was
performed
.
The
result
showed
that
RUNX
3
methylation
was
significantly
higher
in
esophageal
cancer
than
in
normal
squamous
mucosa
from
the
proximal
resection
margin
or
esophageal
benign
lesions
(
OR
 
=
 
2
.
85
,
CI
 
=
 
2
.
01
-
4
.
05
,
P
<
0
.
00001
)
.
The
prevalence
of
lymph
node
involvement
,
tumor
size
(
T
1
-
T
2
vs
T
3
-
T
4
)
and
histological
grade
was
significantly
greater
in
RUNX
3
-
negative
cases
(
RUNX
3
unmethylated
groups
)
than
in
RUNX
3
-
positive
cases
(
OR
 
=
 
0
.
25
,
CI
 
=
 
0
.
14
-
0
.
43
,
P
<
0
.
00001
)
.
RUNX
3
methylation
was
significantly
higher
in
esophageal
adenocarcinoma
(
EAC
)
than
Barrett
's
esophagus
(
OR
 
=
 
0
.
35
,
CI
 
=
 
0
.
20
-
0
.
59
,
P
<
0
.
0001
)
.
In
addition
,
the
pooled
HR
for
overall
survival
(
OS
)
showed
that
decreased
RUNX
3
expression
was
associated
with
worse
survival
in
esophageal
cancer
(
HR
 
=
 
4
.
31
,
95
%
CI
 
=
 
2
.
57
-
7
.
37
,
P
<
0
.
00001
)
.
The
results
of
this
meta
-analysis
suggest
that
RUNX
3
methylation
is
associated
with
an
increased
risk
,
progression
as
well
as
worse
survival
in
esophageal
cancer
.
RUNX
3
methylation
,
which
induces
the
inactivation
of
RUNX
3
gene
,
plays
an
important
role
in
esophageal
carcinogenesis
.
Diseases
Validation
Diseases presenting
"cancer"
symptom
achondroplasia
acute rheumatic fever
adrenal incidentaloma
alpha-thalassemia
benign recurrent intrahepatic cholestasis
cadasil
canavan disease
carcinoma of the gallbladder
cholangiocarcinoma
coats disease
congenital adrenal hyperplasia
congenital diaphragmatic hernia
cowden syndrome
cushing syndrome
cutaneous mastocytosis
dedifferentiated liposarcoma
dystrophic epidermolysis bullosa
epidermolysis bullosa simplex
erdheim-chester disease
erythropoietic protoporphyria
esophageal adenocarcinoma
esophageal carcinoma
esophageal squamous cell carcinoma
familial hypocalciuric hypercalcemia
familial mediterranean fever
gm1 gangliosidosis
heparin-induced thrombocytopenia
hereditary cerebral hemorrhage with amyloidosis
hirschsprung disease
hodgkin lymphoma, classical
inclusion body myositis
junctional epidermolysis bullosa
kabuki syndrome
kallmann syndrome
kindler syndrome
lamellar ichthyosis
liposarcoma
locked-in syndrome
lymphangioleiomyomatosis
monosomy 21
neuralgic amyotrophy
oculocutaneous albinism
oligodontia
oral submucous fibrosis
papillon-lefèvre syndrome
pendred syndrome
pleomorphic liposarcoma
primary effusion lymphoma
proteus syndrome
pyomyositis
pyruvate dehydrogenase deficiency
severe combined immunodeficiency
sneddon syndrome
systemic capillary leak syndrome
triple a syndrome
von hippel-lindau disease
waldenström macroglobulinemia
well-differentiated liposarcoma
werner syndrome
wiskott-aldrich syndrome
wolf-hirschhorn syndrome
x-linked adrenoleukodystrophy
This symptom has already been validated