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Human herpesvirus 8 interleukin-6 contributes to primary effusion lymphoma cell viability via suppression of proapoptotic cathepsin D, a cointeraction partner of vitamin K epoxide reductase complex subunit 1 variant 2.
[primary effusion lymphoma]
Human
herpesvirus
8
(
HHV-
8
)
interleukin-
6
(
vIL-
6
)
promotes
cell
proliferation
and
survival
and
is
proangiogenic
,
implicating
it
as
a
contributor
to
virus-associated
Kaposi
's
sarcoma
,
primary
effusion
lymphoma
(
PEL
)
,
and
multicentric
Castleman
's
disease
.
Although
predominantly
lytically
expressed
,
vIL-
6
is
also
produced
at
low
,
functional
levels
during
latency
in
PEL
cells
.
Unlike
other
IL
-
6
cytokines
,
vIL-
6
is
secreted
very
inefficiently
and
localizes
in
the
endoplasmic
reticulum
(
ER
)
.
ER-
localized
vIL-
6
supports
PEL
cell
proliferation
and
survival
,
mediated
in
part
through
its
interaction
with
the
largely
uncharacterized
ER-resident
protein
vitamin
K
epoxide
reductase
complex
subunit
1
variant
2
(
VKORC
1
v
2
)
.
Here
,
we
report
that
the
ER-transiting
and
functionally
mitogenic
secreted
proenzyme
(
pCatD
)
form
of
cathepsin
D
(
mature
CatD
)
,
a
proapoptotic
lysosomal
aspartate
protease
,
is
an
interaction
partner
of
VKORC
1
v
2
and
that
vIL-
6
promotes
this
interaction
.
Depletion
of
vIL-
6
in
PEL
cells
increased
levels
of
the
catalytically
active
,
proteolytically
cleaved
form
of
CatD
,
corresponding
with
decreased
PEL
cell
viability
.
Ectopic
expression
of
CatD
in
PEL
cells
induced
apoptosis
,
suggesting
that
CatD
suppression
by
vIL-
6
is
biologically
significant
.
In
the
context
of
high
-density
culture
or
reactivation
of
HHV-
8
lytic
replication
in
PEL
cells
,
CatD
depletion
substantially
reduced
stress-induced
apoptosis
and
increased
virus
production
.
In
contrast
,
CatD
overexpression
,
vIL-
6
depletion
,
and
peptide-mediated
disruption
of
vIL-
6
-
VKORC
1
v
2
interaction
inhibited
replication
and
cell
survival
.
Combined
,
our
data
identify
pCatD
as
an
interaction
partner
of
VKORC
1
v
2
,
demonstrate
a
role
of
vIL-
6
in
CatD
suppression
via
VKORC
1
v
2
in
PEL
cells
,
and
identify
a
biologically
significant
mechanism
of
vIL-
6
prosurvival
and
proreplication
activities
via
VKORC
1
v
2
.
Diseases
Validation
Diseases presenting
"increased virus production"
symptom
primary effusion lymphoma
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