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A novel FGFR3-binding peptide inhibits FGFR3 signaling and reverses the lethal phenotype of mice mimicking human thanatophoric dysplasia.
[achondroplasia]
Gain-of-function
mutations
in
fibroblast
growth
factor
receptor-
3
(
FGFR
3
)
lead
to
several
types
of
human
skeletal
dysplasia
syndromes
including
achondroplasia
,
hypochondroplasia
and
thanatophoric
dysplasia
(
TD
)
.
Currently
,
there
are
no
effective
treatments
for
these
skeletal
dysplasia
diseases
.
In
this
study
,
we
screened
,
using
FGFR
3
as
a
bait
,
a
random
12
-
peptide
phage
library
and
obtained
23
positive
clones
that
share
identical
amino
acid
sequences
(
VSPPLTLGQLLS
)
,
named
as
peptide
P
3
.
This
peptide
had
high
binding
specificity
to
the
extracellular
domain
of
FGFR
3
.
P
3
inhibited
tyrosine
kinase
activity
of
FGFR
3
and
its
typical
downstream
molecules
,
extracellular
signal-regulated
kinase
/
mitogen-activated
protein
kinase
.
P
3
also
promoted
proliferation
and
chondrogenic
differentiation
of
cultured
ATDC
5
chondrogenic
cells
.
In
addition
,
P
3
alleviated
the
bone
growth
retardation
in
bone
rudiments
from
mice
mimicking
human
thanatophoric
dysplasia
type
II
(
TDII
)
.
Finally
,
P
3
reversed
the
neonatal
lethality
of
TDII
mice
.
Thus
,
this
study
identifies
a
novel
inhibitory
peptide
for
FGFR
3
signaling
,
which
may
serve
as
a
potential
therapeutic
agent
for
the
treatment
of
FGFR
3
-
related
skeletal
dysplasia
.
Diseases
Validation
Diseases presenting
"also promoted proliferation"
symptom
achondroplasia
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