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The paraproteins in systemic capillary leak syndrome.
[systemic capillary leak syndrome]
Systemic
capillary
leak
syndrome
(
SCLS
)
is
a
rare
disease
characterized
by
episodes
of
collapse
due
to
rapid
transfer
of
considerable
volumes
of
plasma
from
the
intravascular
to
the
extravascular
compartment
.
The
pathogenesis
of
this
disease
is
unknown
.
The
diagnosis
is
made
largely
on
clinical
grounds
,
and
investigations
are
unhelpful
.
The
only
consistent
abnormality
is
that
an
IgG
paraprotein
is
found
in
most
patients
,
raising
the
possibility
that
the
paraprotein
may
be
involved
in
the
pathogenesis
of
the
disease
.
Reduction
of
the
paraprotein
level
in
our
patient
was
associated
with
remission
.
Blood
samples
from
three
SCLS
patients
and
one
probable
SCLS
have
been
studied
.
All
patients
had
monoclonal
IgG
paraproteins
.
The
purified
paraproteins
were
all
of
IgG
1
subclass
and
had
kappa
light
chains
.
However
,
they
differed
in
size
and
charge
.
Antibodies
against
each
of
the
paraproteins
were
raised
in
rabbits
.
Affinity-purified
anti-idiotypic
antibodies
were
tested
for
cross-reactivity
against
the
other
paraproteins
using
immunoblotting
and
Ouchterlony
assay
.
These
assays
showed
that
the
anti-idiotypic
antibodies
reacted
only
with
the
immunizing
paraprotein
and
not
with
any
of
the
other
paraproteins
,
i
.
e
.
that
the
paraproteins
do
not
share
a
common
idiotype
.
Paraproteins
did
not
bind
to
cultured
endothelial
cells
,
either
unactivated
or
following
activation
with
interferon-gamma
(
IFN-gamma
)
,
IL
-
2
or
IL
-
6
.
In
addition
,
we
were
unable
to
demonstrate
any
cytotoxicity
towards
cultured
human
endothelial
cells
by
paraprotein
alone
,
or
in
the
presence
of
neutrophils
(
pronounced
neutrophilia
being
a
feature
of
attacks
)
.
The
relationship
between
the
paraproteins
and
the
disease
remains
unclear
.
It
is
likely
that
additional
,
as
yet
unidentified
,
factors
are
required
for
the
paraprotein
to
lead
to
capillary
leak
.
Diseases
Validation
Diseases presenting
"remission"
symptom
systemic capillary leak syndrome
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