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Altered RIG-I/DDX58-mediated innate immunity in dermatomyositis.
[inclusion body myositis]
We
investigated
the
molecular
mechanisms
involved
in
the
pathogenesis
of
three
inflammatory
myopathies
,
dermatomyositis
(
DM
)
,
polymyositis
(
PM
)
and
inclusion
body
myositis
(
IBM
)
.
We
performed
microarray
experiments
(
â€
)
using
microdissected
pathological
muscle
fibres
from
15
patients
with
these
disorders
and
five
controls
.
Differentially
expressed
candidate
genes
were
validated
by
immunohistochemistry
on
muscle
biopsies
,
and
the
altered
pathways
were
analysed
in
human
myotube
cultures
.
Up-regulation
of
genes
involved
in
viral
and
nucleic
acid
recognition
were
found
in
the
three
myopathies
but
not
in
controls
.
In
DM
,
retinoic
acid-inducible
gene
1
(
RIG-
I
,
DDX
58
)
and
the
novel
antiviral
factor
DDX
60
,
which
promotes
RIG-
I
-mediated
signalling
,
were
significantly
up-regulated
,
followed
by
IFIH
1
(
MDA
5
)
and
TLR
3
.
Immunohistochemistry
confirmed
over-expression
of
RIG-
I
in
pathological
muscle
fibres
in
5
/
5
DM
,
0
/
5
PM
and
0
/
5
IBM
patients
,
and
in
0
/
5
controls
.
Stimulation
of
human
myotubes
with
a
ligand
of
RIG-
I
produced
a
significant
secretion
of
interferon-β
(
IFN
β
;
p
<
0
.
05
)
and
up-regulation
of
class
I
MHC
,
RIG-
I
and
TLR
3
(
p
<
0
.
05
)
by
IFN
β-dependent
and
TLR
3
-
independent
mechanisms
.
RIG-
I
-mediated
innate
immunity
,
triggered
by
a
viral
or
damage
signal
,
plays
a
significant
role
in
the
pathogenesis
of
DM
,
but
not
in
that
of
PM
or
IBM
.
Diseases
Validation
Diseases presenting
"myositis"
symptom
focal myositis
inclusion body myositis
malignant atrophic papulosis
pyomyositis
systemic capillary leak syndrome
This symptom has already been validated