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Screening Newborn Blood Spots for 22q11.2 Deletion Syndrome Using Multiplex Droplet Digital PCR.
[22q11.2 deletion syndrome]
The
diagnosis
of
22
q
11
deletion
syndrome
(
22
q
11
DS
)
is
often
delayed
or
missed
due
to
the
wide
spectrum
of
clinical
involvement
ranging
from
mild
to
severe
,
often
life-threatening
conditions
.
A
delayed
diagnosis
can
lead
to
life-
long
health
issues
that
could
be
ameliorated
with
early
intervention
and
treatment
.
Owing
to
the
high
impact
of
22
q
11
DS
on
public
health
,
propositions
have
been
made
to
include
22
q
11
DS
in
newborn
screening
panels
;
however
,
the
method
of
choice
for
detecting
22
q
11
DS
,
fluorescent
in
situ
hybridization
,
requires
specialized
equipment
and
is
cumbersome
for
most
laboratories
to
implement
as
part
of
their
routine
screening
.
We
sought
to
develop
a
new
genetic
screen
for
22
q
11
DS
that
is
rapid
,
cost-effective
,
and
easily
used
by
laboratories
currently
performing
newborn
screening
.
We
evaluated
the
accuracy
of
multiplex
droplet
digital
PCR
(
ddPCR
)
in
the
detection
of
copy
number
of
22
q
11
DS
by
screening
samples
from
26
patients
with
22
q
11
DS
blindly
intermixed
with
1096
blood
spot
cards
from
the
general
population
(
total
n
=
1122
)
.
Multiplex
ddPCR
correctly
identified
all
22
q
11
DS
samples
and
distinguished
between
1
.
5
-
and
3
-
Mb
deletions
,
suggesting
the
approach
is
sensitive
and
specific
for
the
detection
of
22
q
11
DS
.
These
data
demonstrate
the
utility
of
multiplex
ddPCR
for
large
-scale
population-based
studies
that
screen
for
22
q
11
DS
.
The
use
of
samples
from
blood
spot
cards
suggests
that
this
approach
has
promise
for
newborn
screening
of
22
q
11
DS
,
and
potentially
for
other
microdeletion
syndromes
,
for
which
early
detection
can
positively
impact
clinical
outcome
for
those
affected
.
Diseases
Validation
Diseases presenting
"the wide spectrum of clinical involvement ranging from mild to severe"
symptom
22q11.2 deletion syndrome
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