Rare Diseases Symptoms Automatic Extraction
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A random Abstract
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Single molecule analysis of serotonin transporter regulation using antagonist-conjugated quantum dots reveals restricted, p38 MAPK-dependent mobilization underlying uptake activation.
[gm1 gangliosidosis]
The
presynaptic
serotonin
(
5
-
HT
)
transporter
(
SERT
)
is
targeted
by
widely
prescribed
antidepressant
medications
.
Altered
SERT
expression
or
regulation
has
been
implicated
in
multiple
neuropsychiatric
disorders
,
including
anxiety
,
depression
and
autism
.
Here
,
we
implement
a
generalizable
strategy
that
exploits
antagonist-conjugated
quantum
dots
(
Qdots
)
to
monitor
,
for
the
first
time
,
single
SERT
proteins
on
the
surface
of
serotonergic
cells
.
We
document
two
pools
of
SERT
proteins
defined
by
lateral
mobility
,
one
that
exhibits
relatively
free
diffusion
,
and
a
second
,
localized
to
cholesterol
and
GM
1
ganglioside-enriched
microdomains
,
that
displays
restricted
mobility
.
Receptor-linked
signaling
pathways
that
enhance
SERT
activity
mobilize
transporters
that
,
nonetheless
,
remain
confined
to
membrane
microdomains
.
Mobilization
of
transporters
arises
from
a
p
38
MAPK-dependent
untethering
of
the
SERT
C
terminus
from
the
juxtamembrane
actin
cytoskeleton
.
Our
studies
establish
the
utility
of
ligand-conjugated
Qdots
for
analysis
of
the
behavior
of
single
membrane
proteins
and
reveal
a
physical
basis
for
signaling-mediated
SERT
regulation
.
Diseases
Validation
Diseases presenting
"single sert proteins on the surface of serotonergic cells"
symptom
gm1 gangliosidosis
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