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Molecular mechanism of epigallocatechin-3-gallate in human esophageal squamous cell carcinoma in vitro and in vivo.
[esophageal squamous cell carcinoma]
Epigallocatechin-
3
-
gallate
(
EGCG
)
,
the
major
polyphenol
of
green
tea
,
has
been
shown
to
inhibit
proliferation
in
various
types
of
tumors
.
However
,
few
studies
concerning
the
role
and
mechanism
of
EGCG
in
esophageal
squamous
cell
carcinoma
are
available
.
Therefore
,
the
antitumor
mechanism
of
EGCG
needs
to
be
investigated
.
The
present
study
aimed
to
examine
the
antitumor
effect
of
EGCG
on
the
human
esophageal
squamous
cell
carcinoma
cell
lines
,
Eca-
109
and
Te-
1
,
in
Â
vitro
and
in
Â
vivo
.
Cell
viability
was
assessed
using
the
MTT
assay
and
tumor
formation
and
growth
in
murine
xenograft
models
with
or
without
EGCG
treatment
.
Cell
cycle
analysis
and
levels
of
reactive
oxygen
species
(
ROS
)
were
detected
using
flow
cytometry
.
Apoptosis
was
measured
by
Annexin
/
propidium
iodide
staining
.
Caspase-
3
cleavage
and
vascular
endothelial
growth
factor
(
VEGF
)
expression
were
detected
using
western
blot
analysis
and
immunohistochemistry
in
tumor
cell
lines
and
tumor
xenografts
,
respectively
.
The
results
showed
that
EGCG
inhibited
proliferation
in
the
Eca-
109
and
Te-
1
cells
in
a
time-
Â
and
dose-dependent
manner
.
Tumor
cells
were
arrested
in
the
G
1
Â
phase
and
apoptosis
was
accompanied
by
ROS
production
and
caspase-
3
cleavage
.
In
a
mouse
model
,
EGCG
significantly
inhibited
the
growth
of
Eca-
109
tumors
by
increasing
the
expression
of
cleaved-caspase-
3
and
decreasing
VEGF
protein
levels
.
Taken
together
,
the
results
suggest
that
EGCG
inhibits
proliferation
and
induces
apoptosis
through
ROS
production
,
caspase-
3
activation
,
and
a
decrease
in
VEGF
expression
in
Â
vitro
and
in
Â
vivo
.
Furthermore
,
EGCG
may
have
future
clinical
applications
for
novel
approaches
to
treat
esophageal
squamous
cell
carcinoma
.
Diseases
Validation
Diseases presenting
"tumor xenografts"
symptom
esophageal carcinoma
esophageal squamous cell carcinoma
liposarcoma
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