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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
"mechanisms may affect the length of aganglionosis in hscr subgroups during enteric nervous system"
symptom
hirschsprung disease
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