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Characterisation of the conformational changes in platelet factor 4 induced by polyanions: towards in vitro prediction of antigenicity.
[heparin-induced thrombocytopenia]
Heparin-induced
thrombocytopenia
(
HIT
)
is
the
most
frequent
drug-induced
immune
reaction
affecting
blood
cells
.
Its
antigen
is
formed
when
the
chemokine
platelet
factor
4
(
PF
4
)
complexes
with
polyanions
.
By
assessing
polyanions
of
varying
length
and
degree
of
sulfation
using
immunoassay
and
circular
dichroism
(
CD
)
-
spectroscopy
,
we
show
that
PF
4
structural
changes
resulting
in
antiparallel
β-sheet
content
>
30
%
make
PF
4
/
polyanion
complexes
antigenic
.
Further
,
we
found
that
polyphosphates
(
polyP-
55
)
induce
antigenic
changes
on
PF
4
,
whereas
fondaparinux
does
not
.
We
provide
a
model
suggesting
that
conformational
changes
exposing
antigens
on
PF
4
/
polyanion
complexes
occur
in
the
hairpin
involving
AA
32
-
38
,
which
form
together
with
C-
terminal
AA
(
66
-
70
)
of
the
adjacent
PF
4
monomer
a
continuous
patch
on
the
PF
4
tetramer
surface
,
explaining
why
only
tetrameric
PF
4
molecules
express
"
HIT
antigens
"
.
The
correlation
of
antibody
binding
in
immunoassays
with
PF
4
structural
changes
provides
the
intriguing
possibility
that
CD-spectroscopy
could
become
the
first
antibody-independent
,
in
vitro
method
to
predict
potential
immunogenicity
of
drugs
.
CD-spectroscopy
could
identify
compounds
during
preclinical
drug
development
that
induce
PF
4
structural
changes
correlated
with
antigenicity
.
The
clinical
relevance
can
then
be
specifically
addressed
during
clinical
trials
.
Whether
these
findings
can
be
transferred
to
other
endogenous
proteins
requires
further
studies
.
Diseases
Validation
Diseases presenting
"heparin-induced thrombocytopenia"
symptom
heparin-induced thrombocytopenia
This symptom has already been validated