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A purine scaffold HSP90 inhibitor BIIB021 has selective activity against KSHV-associated primary effusion lymphoma and blocks vFLIP K13-induced NF-κB.
[primary effusion lymphoma]
Kaposi
sarcoma
-associated
herpes
virus
(
KSHV
)
-
associated
primary
effusion
lymphomas
(
PEL
)
have
extremely
poor
prognosis
when
treated
with
conventional
chemotherapy
.
KSHV-encoded
viral
FLICE-inhibitory
protein
(
vFLIP
)
K
13
binds
to
the
IkappaB
kinase
(
IKK
)
complex
to
constitutively
activate
the
NF-κB
pathway
,
which
has
been
shown
to
be
essential
for
the
survival
and
proliferation
of
PEL
cells
.
The
molecular
chaperone
HSP
90
is
a
component
of
the
IKK
complex
and
is
required
for
its
activity
.
We
have
analyzed
the
effect
of
HSP
90
inhibitors
on
the
survival
and
proliferation
of
PEL
cells
and
on
the
activity
of
the
NF-κB
pathway
.
We
show
that
BIIB
021
,
a
purine
scaffold-based
orally
administrable
HSP
90
inhibitor
,
shows
preferential
cytotoxicity
toward
PEL
cells
as
compared
with
non-
PEL
cells
.
The
cytotoxic
effect
of
BIIB
021
against
PEL
was
associated
with
induction
of
cell-cycle
arrest
and
apoptosis
.
BIIB
021
blocked
the
expression
of
a
number
of
cellular
proteins
involved
in
the
regulation
of
cell
cycle
and
apoptosis
.
BIIB
021
also
blocked
constitutive
NF-κB
activity
present
in
PEL
cells
,
in
part
,
by
blocking
the
interaction
of
vFLIP
K
13
with
the
IKK
complex
subunits
.
In
a
xenograft
model
of
PEL
,
BIIB
021
significantly
reduced
tumor
growth
.
BIIB
021
blocks
constitutive
NF-κB
activity
in
PEL
and
shows
preferential
antitumor
activity
against
PEL
in
vitro
and
in
vivo
.
BIIB
021
may
be
a
promising
agent
for
treatment
of
PEL
.
Diseases
Validation
Diseases presenting
"apoptosis"
symptom
22q11.2 deletion syndrome
hodgkin lymphoma, classical
pendred syndrome
primary effusion lymphoma
systemic capillary leak syndrome
waldenström macroglobulinemia
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