Rare Diseases Symptoms Automatic Extraction
Home
A random Abstract
Our Project
Our Team
A genome-wide association study identifies potential susceptibility Loci for hirschsprung disease.
[hirschsprung disease]
Hirschsprung
disease
(
HSCR
)
is
a
congenital
and
heterogeneous
disorder
characterized
by
the
absence
of
intramural
nervous
plexuses
along
variable
lengths
of
the
hindgut
.
Although
RET
is
a
well-established
risk
factor
,
a
recent
genome-
wide
association
study
(
GWAS
)
of
HSCR
has
identified
NRG
1
as
an
additional
susceptibility
locus
.
To
discover
additional
risk
loci
,
we
performed
a
GWAS
of
123
sporadic
HSCR
patients
and
432
unaffected
controls
using
a
large
-scale
platform
with
coverage
of
over
1
million
polymorphic
markers
.
The
result
was
that
our
study
replicated
the
findings
of
RET
-
CSGALNACT
2
-
RASGEF
1
A
genomic
region
(
rawP
 
=
 
5
.
69
×
10
-
19
before
a
Bonferroni
correction
;
corrP
 
=
 
4
.
31
×
10
-
13
after
a
Bonferroni
correction
)
and
NRG
1
as
susceptibility
loci
.
In
addition
,
this
study
identified
SLC
6
A
20
(
adjP
 
=
 
2
.
71
×
10
-
6
)
,
RORA
(
adjP
 
=
 
1
.
26
×
10
-
5
)
,
and
ABCC
9
(
adjP
 
=
 
1
.
86
×
10
-
5
)
as
new
potential
susceptibility
loci
under
adjusting
the
already
known
loci
on
the
RET
-
CSGALNACT
2
-
RASGEF
1
A
and
NRG
1
regions
,
although
none
of
the
SNPs
in
these
genes
passed
the
Bonferroni
correction
.
In
further
subgroup
analysis
,
the
RET
-
CSGALNACT
2
-
RASGEF
1
A
genomic
region
was
observed
to
have
different
significance
levels
among
subgroups
:
short
-segment
(
S-
HSCR
,
corrP
 
=
 
1
.
71
×
10
-
5
)
,
long
-segment
(
L-
HSCR
,
corrP
 
=
 
6
.
66
×
10
-
4
)
,
and
total
colonic
aganglionosis
(
TCA
,
corrP
>
0
.
05
)
.
This
differential
pattern
in
the
significance
level
suggests
that
other
genomic
loci
or
mechanisms
may
affect
the
length
of
aganglionosis
in
HSCR
subgroups
during
enteric
nervous
system
(
ENS
)
development
.
Although
functional
evaluations
are
needed
,
our
findings
might
facilitate
improved
understanding
of
the
mechanisms
of
HSCR
pathogenesis
.
Diseases
Validation
Diseases presenting
"wide association study"
symptom
cadasil
esophageal adenocarcinoma
hirschsprung disease
inclusion body myositis
lamellar ichthyosis
You can validate or delete this automatically detected symptom
Validate the Symptom
Delete the Symptom