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A random Abstract
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Our Team
Evaluation of the therapeutic potential of a CNP analog in a Fgfr3 mouse model recapitulating achondroplasia.
[achondroplasia]
Achondroplasia
(
ACH
)
,
the
most
common
form
of
dwarfism
,
is
an
inherited
autosomal-dominant
chondrodysplasia
caused
by
a
gain-of-function
mutation
in
fibroblast-
growth
-
factor
-receptor
3
(
FGFR
3
)
.
C-
type
natriuretic
peptide
(
CNP
)
antagonizes
FGFR
3
downstream
signaling
by
inhibiting
the
pathway
of
mitogen-activated
protein
kinase
(
MAPK
)
.
Here
,
we
report
the
pharmacological
activity
of
a
39
amino
acid
CNP
analog
(
BMN
111
)
with
an
extended
plasma
half
-life
due
to
its
resistance
to
neutral-endopeptidase
(
NEP
)
digestion
.
In
ACH
human
growth
-plate
chondrocytes
,
we
demonstrated
a
decrease
in
the
phosphorylation
of
extracellular-signal-regulated
kinases
1
and
2
,
confirming
that
this
CNP
analog
inhibits
fibroblast-
growth
-
factor
-mediated
MAPK
activation
.
Concomitantly
,
we
analyzed
the
phenotype
of
Fgfr
3
(
Y
367
C
/
+
)
mice
and
showed
the
presence
of
ACH-related
clinical
features
in
this
mouse
model
.
We
found
that
in
Fgfr
3
(
Y
367
C
/
+
)
mice
,
treatment
with
this
CNP
analog
led
to
a
significant
recovery
of
bone
growth
.
We
observed
an
increase
in
the
axial
and
appendicular
skeleton
lengths
,
and
improvements
in
dwarfism
-related
clinical
features
included
flattening
of
the
skull
,
reduced
crossbite
,
straightening
of
the
tibias
and
femurs
,
and
correction
of
the
growth
-plate
defect
.
Thus
,
our
results
provide
the
proof
of
concept
that
BMN
111
,
a
NEP-resistant
CNP
analog
,
might
benefit
individuals
with
ACH
and
hypochondroplasia
.
Diseases
Validation
Diseases presenting
"dwarfism"
symptom
achondroplasia
gm1 gangliosidosis
kabuki syndrome
lamellar ichthyosis
oculocutaneous albinism
oligodontia
proteus syndrome
This symptom has already been validated