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Combination of SNX-2112 with 5-FU exhibits antagonistic effect in esophageal cancer cells.
[esophageal squamous cell carcinoma]
The
low
efficacy
of
single
-drug
chemotherapy
forms
the
basis
for
combination
therapy
in
esophageal
squamous
cell
carcinoma
.
SNX-
2112
,
a
selective
heat
shock
protein
90
(
Hsp
90
)
inhibitor
,
was
recently
reported
as
being
effective
in
combination
with
cisplatin
and
paclitaxel
.
In
this
study
,
we
investigated
the
effect
of
SNX-
2112
in
combination
with
5
-
fluorouracil
(
5
-
FU
)
,
another
first
-line
anticancer
drug
,
in
esophageal
cancer
.
Unexpectedly
,
tetrazolium
assay
revealed
that
the
combination
of
SNX-
2112
with
5
-
FU
exhibited
antagonistic
effect
.
Flow
cytometry
revealed
that
the
SNX-
2112
and
5
-
FU
combination
greatly
decreased
the
number
of
G
2
/
M
cells
compared
to
SNX-
2112
-
only
treatment
in
Eca‑
109
cells
.
This
effect
might
be
related
to
the
altered
mRNA
level
of
cyclin-related
genes
including
cyclin
Â
D
1
,
Chk
2
and
Cdk
4
.
Further
,
5
-
FU
attenuated
SNX-
2112
-
induced
apoptosis
by
decreasing
poly
(
ADP-ribose
)
polymerase
(
PARP
)
cleavage
and
inactivating
caspase-
3
,
-
8
and
-
9
.
Additionally
,
5
-
FU
suppressed
the
SNX-
2112
-
induced
decrease
of
mitochondrial
membrane
potential
.
Moreover
,
5
-
FU
partly
recovered
Hsp
90
client
proteins
,
including
Akt
,
p
-
Akt
,
inhibitor
of
κB
kinase
(
IKK
)
α
,
extracellular
signal-regulated
kinase
(
ERK
)
1
/
2
,
and
glycogen
synthase
kinase
(
GSK
)
-
3
β
,
which
SNX-
2112
had
downregulated
.
Taken
together
,
this
is
the
first
report
that
the
combination
of
SNX-
2112
with
5
-
FU
exhibited
antagonistic
effect
in
esophageal
cancer
cells
by
affecting
growth
inhibition
,
cell
cycle
,
apoptosis
,
and
Hsp
90
client
proteins
,
suggesting
that
care
is
required
in
the
clinical
application
of
combined
SNX-
2112
and
5
-
FU
.
Diseases
Validation
Diseases presenting
"low efficacy"
symptom
esophageal squamous cell carcinoma
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