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A bioassay for the detection of neutralizing antibodies against the α-melanocyte stimulating hormone analog afamelanotide in patients with erythropoietic protoporphyria.
[erythropoietic protoporphyria]
The
tridecapeptide
afamelanotide
(
Scenesse
®
)
is
a
congener
of
α-melanocyte
stimulating
hormone
(
α-
MSH
)
.
Upon
binding
to
the
melanocortin
1
receptor
(
MC
1
R
)
on
the
surface
of
pigment
cells
of
the
skin
,
the
melanocytes
,
α-
MSH
or
afamelanotide
trigger
the
synthesis
of
cAMP
,
which
stimulates
the
synthesis
of
melanin
and
therefore
induces
skin
tanning
.
In
a
recent
trial
,
afamelanotide
administered
as
controlled
release
implants
protected
erythropoietic
protoporphyria
(
EPP
)
patients
from
sunlight
induced
phototoxic
skin
reactions
.
Administration
of
biological
therapeutic
peptides
may
elicit
unwanted
immunogenic
responses
in
recipients
of
these
products
.
Although
in
a
previous
study
using
ELISA
technique
we
excluded
any
newly
developed
immunogenicity
during
prolonged
exposure
to
afamelanotide
,
we
confirmed
the
previously
published
existence
of
low
titers
of
antibodies
against
α-
MSH
in
drug-naïve
individuals
that
cross-reacted
with
afamelanotide
.
In
order
to
investigate
whether
such
antibodies
are
neutralizing
,
i
.
e
.
could
block
the
biological
effect
of
afamelanotide
,
we
developed
a
cell
culture-based
bioassay
.
The
basis
of
our
assay
was
the
measurement
of
afamelanotide-induced
cAMP
formation
in
a
strain
of
the
B
16
mouse
melanoma
cell
line
,
G
4
F
-
7
,
expressing
the
transfected
human
MC
1
R
.
Average
half
-effective
concentrations
of
the
natural
hormone
α-
MSH
and
its
congener
afamelanotide
were
38
.
8
±
10
.
6
and
10
.
9
±
7
.
17
nM
(
n
=
5
)
,
respectively
.
Neutralizing
antibodies
would
reduce
the
cAMP
formation
.
Two
neutralizing
anti-
α-
MSH
antibodies
served
as
positive
controls
.
cAMP
formation
in
the
G
4
F
-
7
cells
after
addition
of
sera
of
drug-naïve
(
n
=
6
)
and
of
drug-exposed
EPP
patients
(
n
=
17
)
was
significantly
lower
than
after
that
from
healthy
volunteers
(
n
=
13
)
.
There
was
no
difference
between
drug-naïve
and
drug-exposed
patients
.
Using
forskolin
as
a
hormone-independent
stimulator
of
cAMP
formation
,
we
excluded
an
unspecific
interference
of
EPP
sera
with
cAMP
formation
.
We
conclude
that
afamelanotide
even
after
prolonged
application
to
EPP
patients
did
not
elicit
neutralizing
antibodies
.
Further
,
the
low
titer
immunoreactivity
observed
in
sera
of
some
drug-naïve
individuals
had
no
effect
on
the
biological
activity
of
afamelanotide
.
Diseases
Validation
Diseases presenting
"biological therapeutic peptides"
symptom
erythropoietic protoporphyria
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