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Next generation sequencing reveals skewing of the T and B cell receptor repertoires in patients with wiskott-Aldrich syndrome.
[wiskott-aldrich syndrome]
The
Wiskott-
Aldrich
syndrome
(
WAS
)
is
due
to
mutations
of
the
WAS
gene
encoding
for
the
cytoskeletal
WAS
protein
,
leading
to
abnormal
downstream
signaling
from
the
T
cell
and
B
cell
antigen
receptors
(
TCR
and
BCR
)
.
We
hypothesized
that
the
impaired
signaling
through
the
TCR
and
BCR
in
WAS
would
subsequently
lead
to
aberrations
in
the
immune
repertoire
of
WAS
patients
.
Using
next
generation
sequencing
(
NGS
)
,
the
T
cell
receptor
β
and
B
cell
immunoglobulin
heavy
chain
(
IGH
)
repertoires
of
eight
patients
with
WAS
and
six
controls
were
sequenced
.
Clonal
expansions
were
identified
within
memory
CD
4
(
+
)
cells
as
well
as
in
total
,
naïve
and
memory
CD
8
(
+
)
cells
from
WAS
patients
.
In
the
B
cell
compartment
,
WAS
patient
IGH
repertoires
were
also
clonally
expanded
and
showed
skewed
usage
of
IGHV
and
IGHJ
genes
,
and
increased
usage
of
IGHG
constant
genes
,
compared
with
controls
.
To
our
knowledge
,
this
is
the
first
study
that
demonstrates
significant
abnormalities
of
the
immune
repertoire
in
WAS
patients
using
NGS
.
Diseases
Validation
Diseases presenting
"mutations of the was gene encoding for the cytoskeletal was protein"
symptom
wiskott-aldrich syndrome
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