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Molecular biology of human herpesvirus 8: novel functions and virus-host interactions implicated in viral pathogenesis and replication.
[primary effusion lymphoma]
Human
herpesvirus
8
(
HHV-
8
)
,
also
known
as
Kaposi
's
sarcoma
-associated
herpesvirus
(
KSHV
)
,
is
the
second
identified
human
gammaherpesvirus
.
Like
its
relative
Epstein-
Barr
virus
,
HHV-
8
is
linked
to
B-
cell
tumors
,
specifically
primary
effusion
lymphoma
and
multicentric
Castleman
's
disease
,
in
addition
to
endothelial-derived
KS
.
HHV-
8
is
unusual
in
its
possession
of
a
plethora
of
"
accessory
"
genes
and
encoded
proteins
in
addition
to
the
core
,
conserved
herpesvirus
and
gammaherpesvirus
genes
that
are
necessary
for
basic
biological
functions
of
these
viruses
.
The
HHV-
8
accessory
proteins
specify
not
only
activities
deducible
from
their
cellular
protein
homologies
but
also
novel
,
unsuspected
activities
that
have
revealed
new
mechanisms
of
virus-host
interaction
that
serve
virus
replication
or
latency
and
may
contribute
to
the
development
and
progression
of
virus-associated
neoplasia
.
These
proteins
include
viral
interleukin-
6
(
vIL-
6
)
,
viral
chemokines
(
vCCLs
)
,
viral
G
protein-coupled
receptor
(
vGPCR
)
,
viral
interferon
regulatory
factors
(
vIRFs
)
,
and
viral
antiapoptotic
proteins
homologous
to
FLICE
(
FADD
-like
IL
-
1
β
converting
enzyme
)
-
inhibitory
protein
(
FLIP
)
and
survivin
.
Other
HHV-
8
proteins
,
such
as
signaling
membrane
receptors
encoded
by
open
reading
frames
K
1
and
K
15
,
also
interact
with
host
mechanisms
in
unique
ways
and
have
been
implicated
in
viral
pathogenesis
.
Additionally
,
a
set
of
micro-
RNAs
encoded
by
HHV-
8
appear
to
modulate
expression
of
multiple
host
proteins
to
provide
conditions
conducive
to
virus
persistence
within
the
host
and
could
also
contribute
to
HHV-
8
-
induced
neoplasia
.
Here
,
we
review
the
molecular
biology
underlying
these
novel
virus-host
interactions
and
their
potential
roles
in
both
virus
biology
and
virus-associated
disease
.
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primary effusion lymphoma
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