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Exacerbated experimental arthritis in Wiskott-Aldrich syndrome protein deficiency: modulatory role of regulatory B cells.
[wiskott-aldrich syndrome]
Patients
deficient
in
the
cytoskeletal
regulator
Wiskott-
Aldrich
syndrome
protein
(
WASp
)
are
predisposed
to
varied
autoimmunity
,
suggesting
it
has
an
important
controlling
role
in
participating
cells
.
IL
-
10
-
producing
regulatory
B
(
Breg
)
cells
are
emerging
as
important
mediators
of
immunosuppressive
activity
.
In
experimental
,
antigen-induced
arthritis
WASp-
deficient
(
WASp
knockout
[
WAS
KO
]
)
mice
developed
exacerbated
disease
associated
with
decreased
Breg
cells
and
regulatory
T
(
Treg
)
cells
,
but
increased
Th
17
cells
in
knee
-draining
LNs
.
Arthritic
WAS
KO
mice
showed
increased
serum
levels
of
B-
cell-activating
factor
,
while
their
B
cells
were
unresponsive
in
terms
of
B-
cell-activating
factor
induced
survival
and
IL
-
10
production
.
Adoptive
transfer
of
WT
Breg
cells
ameliorated
arthritis
in
WAS
KO
recipients
and
restored
a
normal
balance
of
Treg
and
Th
17
cells
.
Mice
with
B-
cell-
restricted
WASp
deficiency
,
however
,
did
not
develop
exacerbated
arthritis
,
despite
exhibiting
reduced
Breg-
and
Treg-cell
numbers
during
active
disease
,
and
Th
17
cells
were
not
increased
over
equivalent
WT
levels
.
These
findings
support
a
contributory
role
for
defective
Breg
cells
in
the
development
of
WAS
-related
autoimmunity
,
but
demonstrate
that
functional
competence
in
other
regulatory
populations
can
be
compensatory
.
A
properly
regulated
cytoskeleton
is
therefore
important
for
normal
Breg-cell
activity
and
complementation
of
defects
in
this
lineage
is
likely
to
have
important
therapeutic
benefits
.
Diseases
Validation
Diseases presenting
"b-cell-restricted wasp deficiency"
symptom
wiskott-aldrich syndrome
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