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Characterization of mutations in ATP8B1 associated with hereditary cholestasis.
[benign recurrent intrahepatic cholestasis]
Progressive
familial
intrahepatic
cholestasis
(
PFIC
)
and
benign
recurrent
intrahepatic
cholestasis
(
BRIC
)
are
clinically
distinct
hereditary
disorders
.
PFIC
patients
suffer
from
chronic
cholestasis
and
develop
liver
fibrosis
.
BRIC
patients
experience
intermittent
attacks
of
cholestasis
that
resolve
spontaneously
.
Mutations
in
ATP
8
B
1
(
previously
FIC
1
)
may
result
in
PFIC
or
BRIC
.
We
report
the
genomic
organization
of
ATP
8
B
1
and
mutation
analyses
of
180
families
with
PFIC
or
BRIC
that
identified
54
distinct
disease
mutations
,
including
10
mutations
predicted
to
disrupt
splicing
,
6
nonsense
mutations
,
11
small
insertion
or
deletion
mutations
predicted
to
induce
frameshifts
,
1
large
genomic
deletion
,
2
small
inframe
deletions
,
and
24
missense
mutations
.
Most
mutations
are
rare
,
occurring
in
1
-
3
families
,
or
are
limited
to
specific
populations
.
Many
patients
are
compound
heterozygous
for
2
mutations
.
Mutation
type
or
location
correlates
overall
with
clinical
severity
:
missense
mutations
are
more
common
in
BRIC
(
58
%
vs
.
38
%
in
PFIC
)
,
while
nonsense
,
frameshifting
,
and
large
deletion
mutations
are
more
common
in
PFIC
(
41
%
vs
.
16
%
in
BRIC
)
.
Some
mutations
,
however
,
lead
to
a
wide
range
of
phenotypes
,
from
PFIC
to
BRIC
or
even
no
clinical
disease
.
ATP
8
B
1
mutations
were
detected
in
30
%
and
41
%
,
respectively
,
of
the
PFIC
and
BRIC
patients
screened
.
Diseases
Validation
Diseases presenting
"pfic or bric"
symptom
benign recurrent intrahepatic cholestasis
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