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Loss of Tbx1 induces bone phenotypes similar to cleidocranial dysplasia.
[22q11.2 deletion syndrome]
T
-
box
transcription
factor
,
TBX
1
,
is
the
major
candidate
gene
for
22
q
11
.
2
deletion
syndrome
(
DiGeorge
/
Velo-cardio-
facial
syndrome
)
characterized
by
facial
defects
,
thymus
hypoplasia
,
cardiovascular
anomalies
and
cleft
palates
.
Here
,
we
report
that
the
loss
of
Tbx
1
in
mouse
(
Tbx
1
(
-
/
-
)
)
results
in
skeletal
abnormalities
similar
to
those
of
cleidocranial
dysplasia
(
CCD
)
in
humans
,
which
is
an
autosomal-dominant
skeletal
disease
caused
by
mutations
in
RUNX
2
.
Tbx
1
(
-
/
-
)
mice
display
short
stature
,
absence
of
hyoid
bone
,
failed
closure
of
fontanelle
,
bifid
xiphoid
process
and
hypoplasia
of
clavicle
and
zygomatic
arch
.
A
cell-
type
-
specific
deletion
of
Tbx
1
in
osteochondro-progenitor
(
Tbx
1
(
OPKO
)
)
or
mesodermal
(
Tbx
1
(
MKO
)
)
lineage
partially
recapitulates
the
Tbx
1
(
-
/
-
)
bone
phenotypes
.
Although
Tbx
1
expression
has
not
been
previously
reported
in
neural
crest
,
inactivation
of
Tbx
1
in
the
neural
crest
lineage
(
Tbx
1
(
NCKO
)
)
leads
to
an
absence
of
the
body
of
hyoid
bone
and
postnatal
lethality
,
indicating
an
unanticipated
role
of
Tbx
1
in
neural
crest
development
.
Indeed
,
Tbx
1
is
expressed
in
the
neural
crest-derived
hyoid
bone
primordium
,
in
addition
to
mesoderm-derived
osteochondral
progenitors
.
Ablation
of
Tbx
1
affected
Runx
2
expression
in
calvarial
bones
and
overexpression
of
Tbx
1
induced
Runx
2
expression
in
vitro
.
Taken
together
,
our
current
studies
reveal
that
Tbx
1
is
required
for
mesoderm-
and
neural
crest-derived
osteoblast
differentiation
and
normal
skeletal
development
.
TBX
1
mutation
could
lead
to
CCD-like
bone
phenotypes
in
human
.
Diseases
Validation
Diseases presenting
"mutations in runx2"
symptom
22q11.2 deletion syndrome
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