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Identification of multifaceted binding modes for pyrin and ASC pyrin domains gives insights into pyrin inflammasome assembly.
[familial mediterranean fever]
Inflammasomes
are
macromolecular
complexes
that
mediate
inflammatory
and
cell
death
responses
to
pathogens
and
cellular
stress
signals
.
Dysregulated
inflammasome
activation
is
associated
with
autoinflammatory
syndromes
and
several
common
diseases
.
During
inflammasome
assembly
,
oligomerized
cytosolic
pattern
recognition
receptors
recruit
procaspase-
1
and
procaspase-
8
via
the
adaptor
protein
ASC
.
Inflammasome
assembly
is
mediated
by
pyrin
domains
(
PYDs
)
and
caspase
recruitment
domains
,
which
are
protein
interaction
domains
of
the
death
fold
superfamily
.
However
,
the
molecular
details
of
their
interactions
are
poorly
understood
.
We
have
studied
the
interaction
between
ASC
and
pyrin
PYDs
that
mediates
ASC
recruitment
to
the
pyrin
inflammasome
,
which
is
implicated
in
the
pathogenesis
of
familial
Mediterranean
fever
.
We
demonstrate
that
both
the
ASC
and
pyrin
PYDs
have
multifaceted
binding
modes
,
involving
three
sites
on
pyrin
PYD
and
two
sites
on
ASC
PYD
.
Molecular
docking
of
pyrin-
ASC
PYD
complexes
showed
that
pyrin
PYD
can
simultaneously
interact
with
up
to
three
ASC
PYDs
.
Furthermore
,
ASC
PYD
can
self-associate
and
interact
with
pyrin
,
consistent
with
previous
reports
that
pyrin
promotes
ASC
clustering
to
form
a
proinflammatory
complex
.
Finally
,
the
effects
of
familial
Mediterranean
fever
-associated
mutations
,
R
42
W
and
A
89
T
,
on
structural
and
functional
properties
of
pyrin
PYD
were
investigated
.
The
R
42
W
mutation
had
a
significant
effect
on
structure
and
increased
stability
.
Although
the
R
42
W
mutant
exhibited
reduced
interaction
with
ASC
,
it
also
bound
less
to
the
pyrin
B-
box
domain
responsible
for
autoinhibition
and
hence
may
be
constitutively
active
.
Our
data
give
new
insights
into
the
binding
modes
of
PYDs
and
inflammasome
architecture
.
Diseases
Validation
Diseases presenting
"fever"
symptom
22q11.2 deletion syndrome
acute rheumatic fever
alexander disease
allergic bronchopulmonary aspergillosis
canavan disease
carcinoma of the gallbladder
child syndrome
congenital toxoplasmosis
cushing syndrome
cystinuria
dracunculiasis
erdheim-chester disease
esophageal adenocarcinoma
esophageal carcinoma
familial mediterranean fever
focal myositis
hodgkin lymphoma, classical
lamellar ichthyosis
legionellosis
locked-in syndrome
malignant atrophic papulosis
neonatal adrenoleukodystrophy
neuralgic amyotrophy
oculocutaneous albinism
papillon-lefèvre syndrome
pyomyositis
pyruvate dehydrogenase deficiency
scrub typhus
severe combined immunodeficiency
sneddon syndrome
systemic capillary leak syndrome
triple a syndrome
typhoid
waldenström macroglobulinemia
wolf-hirschhorn syndrome
This symptom has already been validated