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Tyrosine phosphorylation of Wiskott-Aldrich syndrome protein (WASP) by Hck regulates macrophage function.
[wiskott-aldrich syndrome]
We
have
shown
previously
that
tyrosine
phosphorylation
of
Wiskott-
Aldrich
syndrome
protein
(
WASP
)
is
important
for
diverse
macrophage
functions
including
phagocytosis
,
chemotaxis
,
podosome
dynamics
,
and
matrix
degradation
.
However
,
the
specific
tyrosine
kinase
mediating
WASP
phosphorylation
is
still
unclear
.
Here
,
we
provide
evidence
that
Hck
,
which
is
predominantly
expressed
in
leukocytes
,
can
tyrosine
phosphorylate
WASP
and
regulates
WASP-mediated
macrophage
functions
.
We
demonstrate
that
tyrosine
phosphorylation
of
WASP
in
response
to
stimulation
with
CX
3
CL
1
or
via
Fcγ
receptor
ligation
were
severely
reduced
in
Hck
(
-
/
-
)
bone
marrow-derived
macrophages
(
BMMs
)
or
in
RAW
/
LR
5
macrophages
in
which
Hck
expression
was
silenced
using
RNA-mediated
interference
(
Hck
shRNA
)
.
Consistent
with
reduced
WASP
tyrosine
phosphorylation
,
phagocytosis
,
chemotaxis
,
and
matrix
degradation
are
reduced
in
Hck
(
-
/
-
)
BMMs
or
Hck
shRNA
cells
.
In
particular
,
WASP
phosphorylation
was
primarily
mediated
by
the
p
61
isoform
of
Hck
.
Our
studies
also
show
that
Hck
and
WASP
are
required
for
passage
through
a
dense
three
-dimensional
matrix
and
transendothelial
migration
,
suggesting
that
tyrosine
phosphorylation
of
WASP
by
Hck
may
play
a
role
in
tissue
infiltration
of
macrophages
.
Consistent
with
a
role
for
this
pathway
in
invasion
,
WASP
(
-
/
-
)
BMMs
do
not
invade
into
tumor
spheroids
with
the
same
efficiency
as
WT
BMMs
and
cells
expressing
phospho-
deficient
WASP
have
reduced
ability
to
promote
carcinoma
cell
invasion
.
Altogether
,
our
results
indicate
that
tyrosine
phosphorylation
of
WASP
by
Hck
is
required
for
proper
macrophage
functions
.
Diseases
Validation
Diseases presenting
"specific tyrosine kinase"
symptom
wiskott-aldrich syndrome
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