Rare Diseases Symptoms Automatic Extraction
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Follow-up study of 22 Chinese children with Alexander disease and analysis of parental origin of de novo GFAP mutations.
[alexander disease]
To
delineate
the
phenotype
and
genotype
in
Chinese
children
with
type
I
Alexander
disease
(
AxD
)
and
the
parental
origin
of
de
novo
glial
fibrillary
acidic
protein
(
GFAP
)
mutations
.
Twenty
-
two
children
with
clinically
diagnosed
type
I
AxD
were
followed
up
for
1
.
66
-
6
.
62
years
.
Allele-
specific
PCR
was
used
for
the
analysis
of
parental
origin
of
the
allele
harboring
the
de
novo
mutation
.
Phenotype
of
these
patients
were
consistent
with
type
I
AxD
described
in
other
population
,
with
developmental
delay
(
motor
delay
in
81
.
82
%
,
cognitive
delay
in
63
.
64
%
)
,
macrocephaly
(
100
%
)
,
seizures
(
95
.
45
%
)
,
paroxysmal
deterioration
(
27
.
27
%
)
and
typical
brain
magnetic
resonance
imaging
(
100
%
)
.
Progression
was
slower
than
reported
.
At
8
.
55
years
of
age
(
5
.
29
-
13
.
25
)
,
all
patients
who
underwent
the
second
follow-up
were
alive
.
Eleven
heterozygous
missense
mutations
of
GFAP
were
identified
in
21
patients
,
with
three
novel
mutations
.
Reported
hot
spot
mutations
,
p
.
R
79
,
p
.
R
239
and
p
.
R
88
,
were
also
identified
in
Chinese
patients
.
Mutations
were
de
novo
in
all
but
one
case
.
The
mother
of
a
proband
was
demonstrated
to
be
a
presymptomatic
patient
with
type
II
AxD
with
a
p
.
R
79
H
mutation
.
Ninety
percent
of
de
novo
mutations
were
on
the
paternal
allele
demonstrated
by
allele-
specific
PCR
.
This
is
the
largest
follow-up
study
on
Chinese
children
with
AxD
.
The
phenotypes
of
these
patients
are
consistent
with
reports
in
other
populations
.
GFAP
mutations
were
identified
in
95
.
46
%
of
Chinese
children
with
clinically
diagnosed
type
I
AxD
.
Our
data
suggested
a
male
germ-line
transmission
.
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