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Duplication at Xq13.3-q21.1 with syndromic intellectual disability, a probable role for the ATRX gene.
[alpha-thalassemia]
Here
we
report
on
two
unrelated
male
patients
with
syndromic
intellectual
disability
(
ID
)
due
to
duplication
at
Xq
13
.
3
-
q
21
.
1
,
a
region
of
about
6
 
Mb
and
25
genes
.
Among
these
,
the
most
outstanding
is
ATRX
,
the
causative
gene
of
X-
linked
alpha-thalassemia
/
mental
retardation
.
ATRX
belongs
to
the
growing
list
of
genes
implied
in
chromatin
remodeling
causing
ID
.
Many
these
genes
,
such
as
MECP
2
,
are
dose-sensitive
so
that
not
only
deletions
and
point
mutations
,
but
also
duplications
cause
ID
.
Both
patients
have
severe
ID
,
absent
expressive
speech
,
early
hypotonia
,
behavior
problems
(
hyperactivity
,
repetitive
self-stimulatory
behavior
)
,
postnatal
growth
deficiency
,
microcephaly
,
micrognathia
,
cryptorchidism
,
low
-set
,
posteriorly
angulated
ears
,
and
downslanting
palpebral
fissures
.
These
findings
are
also
usually
present
among
patients
with
loss
-of-function
mutations
of
the
ATRX
gene
.
Completely
skewed
X
inactivation
was
observed
in
the
only
informative
carrier
mother
,
a
constant
finding
among
female
carriers
of
inactivating
point
mutations
of
this
gene
.
Participation
of
other
duplicated
genes
can
not
be
excluded
;
nevertheless
we
propose
that
the
increased
dosage
of
ATRX
is
the
major
pathogenic
mechanism
of
this
X-
linked
disorder
,
a
syndrome
reminiscent
of
MECP
2
duplication
.
Diseases
Validation
Diseases presenting
"early hypotonia"
symptom
alpha-thalassemia
wolf-hirschhorn syndrome
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