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Microarray analysis of unbalanced translocation in Wolf-Hirschhorn syndrome.
[wolf-hirschhorn syndrome]
Wolf-
Hirschhorn
syndrome
(
WHS
)
is
caused
by
deletions
involving
chromosome
region
4
p
16
.
3
,
which
is
characterized
by
growth
delay
,
mild
-
to
-
severe
mental
retardation
,
hypotonia
,
facial
dysmorphisms
and
shows
extensive
phenotypic
variability
include
feeding
difficulties
,
epilepsy
and
congenital
anomalies
.
Variation
in
the
size
of
the
deletion
involving
chromosome
region
4
p
16
.
3
may
explain
the
clinical
variation
.
However
,
previous
studies
indicate
that
duplication
for
another
chromosome
region
due
to
an
unbalanced
translocation
elucidate
approximately
40
-
45
%
WHS
patients
.
Therefore
,
we
used
whole
genomic
cytogenetics
array
to
analyze
the
entire
genome
at
a
significantly
higher
resolution
over
conventional
cytogenetics
to
characterize
the
exact
subtelomeric
aberration
region
of
one
patient
with
developmental
delay
and
several
facial
characteristics
reminiscent
Wolf-
Hirschhorn
syndrome
.
Here
we
report
that
our
patient
had
3
.
7
Mb
deletion
at
the
4
p
16
.
2
and
6
.
8
Mb
duplication
at
8
p
23
.
1
resulted
from
the
unbalanced
translocations
der
(
4
)
t
(
4
;
8
)
(
p
16
.
2
;
p
23
.
1
)
.
We
confirmed
that
our
patient
with
monosomy
4
p
16
.
2
which
is
consistent
with
Wolf-
Hirschhorn
syndrome
and
trisomy
8
p
23
.
1
.
The
combination
of
the
4
p
deletion
with
8
p
partial
trisomy
explains
the
complex
phenotype
presented
by
our
patient
.
Diseases
Validation
Diseases presenting
"developmental delay"
symptom
22q11.2 deletion syndrome
achondroplasia
alexander disease
alpha-thalassemia
aniridia
canavan disease
child syndrome
classical phenylketonuria
coats disease
cohen syndrome
congenital diaphragmatic hernia
congenital toxoplasmosis
cowden syndrome
gm1 gangliosidosis
harlequin ichthyosis
hirschsprung disease
holt-oram syndrome
homocystinuria without methylmalonic aciduria
kabuki syndrome
kallmann syndrome
krabbe disease
lamellar ichthyosis
monosomy 21
neonatal adrenoleukodystrophy
phenylketonuria
primary hyperoxaluria type 1
proteus syndrome
pyruvate dehydrogenase deficiency
sneddon syndrome
triple a syndrome
wolf-hirschhorn syndrome
zellweger syndrome
This symptom has already been validated
