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Antibodies to glutamate receptor subtype 3 (GluR3) are found in some patients suffering from epilepsy as the main disease, but not in patients whose epilepsy accompanies antiphospholipid syndrome or Sneddon's syndrome.
[sneddon syndrome]
Autoantibodies
(
Ab
's
)
to
the
"
B
"
peptide
(
amino
acids
372
-
395
)
of
glutamate
/
AMPA
receptor
subtype
3
(
GluR
3
)
are
found
in
serum
and
cerebrospinal
fluid
of
some
patients
with
different
types
of
epilepsy
.
Since
such
anti-
GluR
3
B
Ab
's
can
activate
and
/
or
kill
neurons
in
vitro
and
in
vivo
,
they
may
contribute
to
epilepsy
.
To
investigate
whether
anti-
GluR
3
B
Ab
's
may
also
be
relevant
to
epilepsy
when
it
accompanies
some
autoimmune
-diseases
,
we
tested
for
these
Ab
's
in
patients
suffering
from
epilepsy
that
accompanies
anti-phospholipid
syndrome
(
APS
)
or
Sneddon
's
syndrome
(
SNS
)
,
both
being
autoimmune
-diseases
with
frequent
neurological
complications
.
We
tested
77
pediatric
patients
whose
epilepsy
is
their
main
disease
;
31
adult
patients
whose
epilepsy
accompanies
APS
(
primary
or
SLE-associated
)
or
SNS
;
45
epilepsy
-free
APS
and
SNS
patients
;
and
90
healthy
controls
.
Compared
to
the
controls
,
significantly
elevated
anti-
GluR
3
B
Ab
's
were
found
in
22
/
77
(
29
%
)
patients
whose
epilepsy
is
their
main
disease
,
but
in
none
of
the
patients
whose
seizures
accompany
APS
or
SNS
.
Yet
,
all
the
APS
and
SNS
patients
harbored
the
characteristic
anti-phospholipid
Ab
's
(
aPL
)
,
directed
against
cardiolipin
and
beta
2
-
glycoprotein
I
,
and
had
lupus
anti-coagulant
.
Thus
,
anti-
GluR
3
B
Ab
's
are
not
crossreactive
with
aPL
,
and
not
produced
as
a
non-
specific
consequence
of
seizures
on
the
one
hand
,
or
autoimmune
-diseases
on
the
other
.
Taken
together
with
new
findings
accumulated
recently
in
our
lab
,
we
suggest
that
anti-
GluR
3
B
Ab
's
are
produced
primarily
in
the
periphery
due
to
specific
/
non-
specific
"
irritation
"
of
the
immune
system
,
and
that
once
they
reach
the
brain
via
a
leaky
blood
-
brain
barrier
they
may
cause
neuronal
/
glial
damage
and
facilitate
the
outburst
of
epilepsy
and
additional
neurological
abnormalities
.
In
contrast
,
the
presence
of
anti-
GluR
3
B
Ab
's
does
not
seem
to
increase
the
probability
of
developing
APS
,
SNS
or
the
seizures
that
often
accompany
these
autoimmune
-diseases
.
These
findings
may
have
important
diagnostic
and
therapeutic
implications
.
Diseases
Validation
Diseases presenting
"specific/non"
symptom
sneddon syndrome
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