Rare Diseases Symptoms Automatic Extraction
Home
A random Abstract
Our Project
Our Team
Structural abnormalities in cortical volume, thickness, and surface area in 22q11.2 microdeletion syndrome: Relationship with psychotic symptoms.
[22q11.2 deletion syndrome]
22
q
11
.
2
deletion
syndrome
(
22
q
11
DS
)
represents
one
of
the
largest
known
genetic
risk
factors
for
psychosis
,
yet
the
neurobiological
mechanisms
underlying
symptom
development
are
not
well
understood
.
Here
we
conducted
a
cross-sectional
study
of
22
q
11
DS
to
decompose
cortical
volume
into
its
constituent
parts
,
cortical
thickness
(
CT
)
and
surface
area
(
SA
)
,
which
are
believed
to
have
distinct
neurodevelopmental
origins
.
High
-resolution
T
1
-
weighted
scans
were
collected
on
65
participants
(
31
22
q
11
DS
,
34
demographically
comparable
typically
developing
controls
,
10
-
25
Â
years
old
)
.
Measures
of
cortical
volume
,
CT
,
and
SA
were
extracted
from
regions
of
interest
using
the
FreeSurfer
image
analysis
suite
.
Group
differences
and
age-related
trajectories
in
these
structures
,
as
well
as
their
association
with
psychotic
symptomatology
,
were
assessed
.
Relative
to
controls
,
22
q
11
DS
participants
showed
bilateral
volumetric
reductions
in
the
inferior
temporal
cortex
,
fusiform
gyrus
,
anterior
cingulate
,
superior
parietal
cortex
,
and
cuneus
,
which
were
driven
by
decreased
SA
in
these
regions
.
22
q
11
DS
participants
also
had
increased
volumes
,
driven
by
increased
CT
,
in
bilateral
insula
regions
.
22
q
11
DS
youth
had
increased
CT
in
frontal
regions
,
particularly
middle
frontal
and
medial
orbitofrontal
cortices
.
A
pattern
of
age-associated
cortical
thinning
was
observed
in
typically
developing
controls
in
brain
regions
associated
with
visual
and
sensory
information-processing
(
i
.
e
.
,
left
pericalcarine
cortex
and
fusiform
gyrus
,
right
lingual
and
postcentral
cortices
)
.
However
,
this
relationship
was
disrupted
in
22
q
11
DS
participants
.
Finally
,
correlational
analyses
revealed
that
increased
CT
in
right
medial
orbitofrontal
cortex
was
associated
with
increased
positive
symptom
severity
in
22
q
11
DS
.
Differential
disruptions
of
CT
and
SA
in
distinct
cortical
regions
in
22
q
11
DS
may
indicate
abnormalities
in
distinct
developmental
neural
processes
.
Further
,
neuroanatomic
abnormalities
in
medial
frontal
brain
structures
disproportionately
affected
in
idiopathic
schizophrenia
were
associated
with
psychotic
symptom
severity
in
22
q
11
DS
youth
,
suggesting
that
disrupted
biological
processes
in
these
cortical
regions
may
underlie
development
of
psychotic
symptoms
,
both
in
22
q
11
DS
and
in
the
broader
population
.
Diseases
Validation
Diseases presenting
"age-related trajectories in these structures"
symptom
22q11.2 deletion syndrome
You can validate or delete this automatically detected symptom
Validate the Symptom
Delete the Symptom