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Association between early-onset Parkinson disease and 22q11.2 deletion syndrome: identification of a novel genetic form of Parkinson disease and its clinical implications.
[22q11.2 deletion syndrome]
Clinical
case
reports
of
parkinsonism
co
-occurring
with
hemizygous
22
q
11
.
2
deletions
and
the
associated
multisystem
syndrome
,
22
q
11
.
2
deletion
syndrome
(
22
q
11
.
2
DS
)
,
suggest
that
22
q
11
.
2
deletions
may
lead
to
increased
risk
of
early
-onset
Parkinson
disease
(
PD
)
.
The
frequency
of
PD
and
its
neuropathological
presentation
remain
unknown
in
this
common
genetic
condition
.
To
evaluate
a
possible
association
between
22
q
11
.
2
deletions
and
PD
.
An
observational
study
of
the
occurrence
of
PD
in
the
world
's
largest
cohort
of
well-characterized
adults
with
a
molecularly
confirmed
diagnosis
of
22
q
11
.
2
DS
(
n
=
159
[
6
with
postmortem
tissue
]
;
age
range
,
18
.
1
-
68
.
6
years
)
was
conducted
in
Toronto
,
Ontario
,
Canada
.
Rare
postmortem
brain
tissue
from
individuals
with
22
q
11
.
2
DS
and
a
clinical
history
of
PD
was
investigated
for
neurodegenerative
changes
and
compared
with
that
from
individuals
with
no
history
of
a
movement
disorder
.
A
clinical
diagnosis
of
PD
made
by
a
neurologist
and
neuropathological
features
of
PD
.
RESULTS
Adults
with
22
q
11
.
2
DS
had
a
significantly
elevated
occurrence
of
PD
compared
with
standard
population
estimates
(
standardized
morbidity
ratio
=
69
.
7
;
95
%
CI
,
19
.
0
-
178
.
5
)
.
All
cases
showed
early
onset
and
typical
PD
symptom
pattern
,
treatment
response
,
and
course
.
All
were
negative
for
family
history
of
PD
and
known
pathogenic
PD-related
mutations
.
The
common
use
of
antipsychotics
in
patients
with
22
q
11
.
2
DS
to
manage
associated
psychiatric
symptoms
delayed
diagnosis
of
PD
by
up
to
10
years
.
Postmortem
brain
tissue
revealed
classic
loss
of
midbrain
dopaminergic
neurons
in
all
3
postmortem
22
q
11
.
2
DS
-PD
cases
.
Typical
α-synuclein-
positive
Lewy
bodies
were
present
in
the
expected
distribution
in
2
cases
but
absent
in
another
.
These
findings
suggest
that
22
q
11
.
2
deletions
represent
a
novel
genetic
risk
factor
for
early
-onset
PD
with
variable
neuropathological
presentation
reminiscent
of
LRRK
2
-
associated
PD
neuropathology
.
Individuals
with
early
-onset
PD
and
classic
features
of
22
q
11
.
2
DS
should
be
considered
for
genetic
testing
,
and
those
with
a
known
22
q
11
.
2
deletion
should
be
monitored
for
the
development
of
parkinsonian
symptoms
.
Molecular
studies
of
the
implicated
genes
,
including
DGCR
8
,
may
help
shed
light
on
the
underlying
pathophysiology
of
PD
in
22
q
11
.
2
DS
and
idiopathic
PD
.
Diseases
Validation
Diseases presenting
"common use"
symptom
22q11.2 deletion syndrome
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