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In vivo composition of NMDA receptor signaling complexes differs between membrane subdomains and is modulated by PSD-95 and PSD-93.
[gm1 gangliosidosis]
Lipid
rafts
are
dynamic
membrane
microdomains
enriched
in
cholesterol
and
sphingolipids
involved
in
the
compartmentalization
of
signaling
pathways
,
trafficking
and
sorting
of
proteins
.
At
synapses
,
the
glutamatergic
NMDA
receptor
and
its
cytoplasmic
scaffold
protein
PSD
-
95
move
between
postsynaptic
density
(
PSD
)
and
rafts
following
learning
or
ischemia
.
However
it
is
not
known
whether
the
signaling
complexes
formed
by
these
proteins
are
different
in
rafts
nor
the
molecular
mechanisms
that
govern
their
localization
.
To
examine
these
issues
in
vivo
we
used
mice
carrying
genetically
encoded
tags
for
purification
of
protein
complexes
and
specific
mutations
in
NMDA
receptors
,
PSD
-
95
and
other
postsynaptic
scaffold
proteins
.
Isolation
of
PSD
-
95
complexes
from
mice
carrying
tandem
affinity
purification
tags
showed
differential
composition
in
lipid
rafts
,
postsynaptic
density
and
detergent-soluble
fractions
.
Raft
PSD
-
95
complexes
showed
less
CaMKIIalpha
and
SynGAP
and
enrichment
in
Src
and
Arc
/
Arg
3
.
1
compared
with
PSD
complexes
.
Mice
carrying
knock-outs
of
PSD
-
95
or
PSD
-
93
show
a
key
role
for
PSD
-
95
in
localizing
NR
2
A
-
containing
NMDA
receptor
complexes
to
rafts
.
Deletion
of
the
NR
2
A
C
terminus
or
the
C-
terminal
valine
residue
of
NR
2
B
,
which
prevents
all
PDZ
interactions
,
reduced
the
NR
1
association
with
rafts
.
Interestingly
,
the
deletion
of
the
NR
2
B
valine
residue
increased
the
total
amount
of
lipid
rafts
.
These
data
show
critical
roles
for
scaffold
proteins
and
their
interactions
with
NMDA
receptor
subunits
in
organizing
the
differential
expression
in
rafts
and
postsynaptic
densities
of
synaptic
signaling
complexes
.
Diseases
Validation
Diseases presenting
"psd-95 and other postsynaptic scaffold proteins"
symptom
gm1 gangliosidosis
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