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The FIC1 gene: structure and polymorphisms in baboon.
[benign recurrent intrahepatic cholestasis]
A
genome
scan
performed
on
648
pedigreed
baboons
to
detect
and
localize
quantitative
trait
loci
(
QTL
)
for
lipoprotein
phenotypes
that
are
known
risk
factors
for
atherosclerosis
indicated
the
presence
of
a
QTL
on
chromosome
18
q
that
exerts
a
major
influence
on
HDL-cholesterol
(
HDL-C
)
related
phenotypes
.
Inspection
of
the
human
gene
map
revealed
that
the
familial
intrahepatic
cholestatis
gene
1
(
FIC
1
)
maps
to
the
homologous
region
of
baboon
chromosome
18
containing
the
major
QTL
influencing
HDL-C
phenotypes
.
FIC
1
is
a
strong
biological
candidate
for
this
QTL
because
HDL-C
is
the
preferred
precursor
for
bile
acid
synthesis
.
In
this
study
,
we
cloned
and
sequenced
FIC
1
cDNA
and
found
that
it
is
highly
conserved
between
human
and
baboon
.
We
also
sequenced
FIC
1
cDNAs
from
a
panel
of
unrelated
baboons
revealing
single
nucleotide
polymorphisms
(
SNPs
)
and
a
polymorphic
dinucleotide
repeat
.
None
of
the
baboon
SNPs
corresponded
to
human
FIC
1
mutations
associated
with
familial
intrahepatic
cholestasis
or
benign
recurrent
intrahepatic
cholestasis
disorders
.
Diseases
Validation
Diseases presenting
"strong biological candidate"
symptom
benign recurrent intrahepatic cholestasis
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