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[Progressive familial intrahepatic cholestasis and hereditary anomalies lf hepatocellular metabolism of bile acids].
[benign recurrent intrahepatic cholestasis]
Progressive
familial
intrahepatic
cholestasis
(
PFIC
)
,
also
known
as
Byler
disease
,
is
an
inherited
cholestasis
of
hepatocellular
origin
which
is
characterized
by
cholestasis
presenting
often
in
the
neonatal
period
leading
to
death
due
to
liver
failure
at
ages
ranging
from
infancy
to
adolescence
.
The
pattern
of
appearance
of
affected
children
within
families
is
consistent
with
autosomal
recessive
inheritance
.
The
etiology
is
poorly
understood
but
several
studies
have
recently
provided
support
for
an
heterogeneity
with
at
least
three
subcategories
among
the
spectrum
of
PFIC
.
The
first
subtype
is
characterized
by
an
early
onset
,
often
during
the
neonatal
period
,
a
severe
pruritus
,
normal
serum
gamma-glutamyltransferase
(
GGT
)
activity
and
cholesterol
level
,
high
concentration
of
serum
primary
bile
acids
,
absence
or
very
low
levels
of
primary
bile
acids
,
absence
or
very
low
levels
of
primary
bile
acids
in
bile
,
and
absence
of
ductular
proliferation
on
standard
optical
liver
histology
.
Its
leads
to
death
due
to
liver
failure
within
a
few
years
,
rarely
after
adolescence
.
It
is
possibly
due
to
an
inborn
error
in
primary
bile
acid
secretion
and
recently
,
a
locus
for
this
subtype
has
been
mapped
in
the
original
Byler
pedigree
to
18
q
21
-
q
22
,
the
benign
recurrent
intrahepatic
cholestasis
region
.
In
the
second
subtype
,
affected
children
exhibit
also
normal
serum
GGT
activity
and
cholesterol
level
and
absence
of
ductular
proliferation
,
but
have
no
pruritus
and
only
traces
of
primary
bile
acids
in
serum
.
An
inborn
error
in
primary
bile
acid
synthesis
has
been
demonstrated
in
this
subtype
.
The
third
subtype
presents
later
in
life
,
carries
a
higher
risk
of
portal
hypertension
and
gastrointestinal
bleeding
and
ends
in
liver
failure
at
a
later
age
.
It
is
characterized
by
a
mild
and
unconstant
pruritus
,
high
GGT
serum
activity
,
moderately
raised
concentrations
of
serum
primary
bile
acids
,
normal
concentration
of
biliary
primary
bile
acids
,
and
ductular
proliferation
and
inflammatory
infiltrate
with
patency
of
intra
and
extrahepatic
bile
ducts
.
An
abnormal
expression
of
the
MDR
3
gene
is
involved
.
A
fair
proportion
of
children
affected
with
all
subtypes
of
PFIC
may
benefit
from
oral
bile
acid
therapy
.
In
some
cases
partial
external
biliary
diversion
or
liver
transplantation
should
be
proposed
.
Diseases
Validation
Diseases presenting
"early onset"
symptom
22q11.2 deletion syndrome
alexander disease
alpha-thalassemia
benign recurrent intrahepatic cholestasis
cadasil
canavan disease
coats disease
cohen syndrome
congenital diaphragmatic hernia
dystrophic epidermolysis bullosa
epidermolysis bullosa simplex
erythropoietic protoporphyria
fabry disease
familial mediterranean fever
homocystinuria without methylmalonic aciduria
inclusion body myositis
kindler syndrome
krabbe disease
papillon-lefèvre syndrome
primary hyperoxaluria type 1
pyruvate dehydrogenase deficiency
scrub typhus
sneddon syndrome
triple a syndrome
von hippel-lindau disease
werner syndrome
wolf-hirschhorn syndrome
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