Inhibition of toxic metal-alpha synuclein interactions by human serum albumin
Chemical Science,
Год журнала:
2024,
Номер
15(10), С. 3502 - 3515
Опубликована: Янв. 1, 2024
Human
serum
albumin
(HSA)
not
only
serves
as
a
crucial
carrier
of
various
ligands
but
also
modulates
the
aggregation
amyloidogenic
proteins,
including
alpha
synuclein
(αSyn),
which
is
associated
with
Parkinson's
disease
and
other
synucleinopathies.
Язык: Английский
Exosomes as Biomarkers and Therapeutic Agents in Neurodegenerative Diseases: Current Insights and Future Directions
Sam Dehghani,
Ozgecan Ocakcı,
Pars Tan Hatipoglu
и другие.
Molecular Neurobiology,
Год журнала:
2025,
Номер
unknown
Опубликована: Март 17, 2025
Abstract
Neurodegenerative
diseases
(NDs)
like
Alzheimer’s,
Parkinson’s,
and
ALS
rank
among
the
most
challenging
global
health
issues,
marked
by
substantial
obstacles
in
early
diagnosis
effective
treatment.
Current
diagnostic
techniques
frequently
demonstrate
inadequate
sensitivity
specificity,
whilst
conventional
treatment
strategies
encounter
challenges
related
to
restricted
bioavailability
insufficient
blood–brain
barrier
(BBB)
permeability.
Recently,
exosomes—nanoscale
vesicles
packed
with
proteins,
RNAs,
lipids—have
emerged
as
promising
agents
potential
reshape
therapeutic
approaches
these
diseases.
Unlike
drug
carriers,
they
naturally
traverse
BBB
can
deliver
bioactive
molecules
affected
neural
cells.
Their
molecular
cargo
influence
cell
signaling,
reduce
neuroinflammation,
potentially
slow
neurodegenerative
progression.
Moreover,
exosomes
serve
non-invasive
biomarkers,
enabling
precise
while
allowing
real-time
disease
monitoring.
Additionally,
engineered
exosomes,
loaded
molecules,
enhance
this
capability
targeting
diseased
neurons
overcoming
barriers.
By
offering
enhanced
reduced
immunogenicity,
an
ability
bypass
physiological
limitations,
exosome-based
present
a
transformative
advantage
over
existing
approaches.
This
review
examines
multifaceted
role
of
NDDs,
emphasizing
their
capabilities,
intrinsic
functions,
advanced
vehicles.
Язык: Английский
Salt-Induced Membrane-Bound Conformation of the NAC Domain of α-Synuclein Leads to Structural Polymorphism of Amyloid Fibrils
Biomolecules,
Год журнала:
2025,
Номер
15(4), С. 506 - 506
Опубликована: Март 31, 2025
α-Synuclein
(αS)
interacts
with
lipid
membranes
in
neurons
to
form
amyloid
fibrils
that
contribute
Parkinson's
disease,
and
its
non-amyloid-β
component
domain
is
critical
the
fibrillation.
In
this
study,
salt
(NaCl)
effect
on
membrane
interaction
fibril
formation
of
αS57-102
peptide
(containing
domain)
was
characterized
at
molecular
level
because
exhibited
structural
polymorphism
two
morphologies
(thin
thick)
presence
NaCl
but
showed
one
morphology
(thin)
absence
NaCl.
The
membrane-bound
conformation
(before
fibrillation)
had
helical
regions
(first
second)
regardless
salt,
length
first
region
largely
shortened
when
present,
exposing
hydrophobic
area
solvent.
exposed
induced
distinct
pathways
nucleation,
depending
molar
ratios
free
αS57-102:
from
association
other
assembly
among
αS57-102.
differences
mainly
affected
β-strand
orientation
content
within
conformations,
probably
contributing
thickness
degree,
leading
polymorphism.
Язык: Английский
Toward a molecular mechanism for the interaction of ATP with alpha-synuclein
Chemical Science,
Год журнала:
2023,
Номер
14(36), С. 9933 - 9942
Опубликована: Янв. 1, 2023
The
ability
of
Adenosine
Triphosphate
(ATP)
to
modulate
protein
solubility
establishes
a
critical
link
between
ATP
homeostasis
and
proteinopathies,
such
as
Parkinson's
(PD).
most
significant
risk
factor
for
PD
is
aging,
levels
decline
dramatically
with
age.
However,
the
mechanism
by
which
interacts
alpha-synuclein
(αS),
whose
aggregation
characteristic
PD,
currently
not
fully
understood,
ATP's
effect
on
αS
aggregation.
Here,
we
use
nuclear
magnetic
resonance
spectroscopy
well
fluorescence,
dynamic
light
scattering
microscopy
show
that
affects
multiple
species
in
self-association
cascade.
triphosphate
moiety
disrupts
long-range
electrostatic
intramolecular
contacts
monomers
enhance
initial
aggregation,
while
also
inhibiting
formation
late-stage
β-sheet
fibrils
disrupting
monomer-fibril
interactions.
These
effects
are
modulated
magnesium
ions
early
onset
PD-related
mutations,
suggesting
loss
hydrotropic
function
fibrillization
may
play
role
etiology.
Язык: Английский
Reply to Matters Arising: In vivo effects of the alpha-synuclein misfolding inhibitor minzasolmin supports clinical development in Parkinson’s disease
npj Parkinson s Disease,
Год журнала:
2024,
Номер
10(1)
Опубликована: Март 14, 2024
Язык: Английский
α-Synuclein and Mitochondria: Probing the Dynamics of Disordered Membrane-protein Regions Using Solid-State Nuclear Magnetic Resonance
JACS Au,
Год журнала:
2024,
Номер
4(6), С. 2372 - 2380
Опубликована: Май 28, 2024
The
characterization
of
intrinsically
disordered
regions
(IDRs)
in
membrane-associated
proteins
is
crucial
importance
to
elucidate
key
biochemical
processes,
including
cellular
signaling,
drug
targeting,
or
the
role
post-translational
modifications.
These
protein
pose
significant
challenges
powerful
analytical
techniques
molecular
structural
investigations.
We
here
applied
magic
angle
spinning
solid-state
nuclear
magnetic
resonance
quantitatively
probe
dynamics
IDRs
membrane-bound
α-synuclein
(αS),
a
whose
aggregation
associated
with
Parkinson's
disease
(PD).
focused
on
mitochondrial
binding
αS,
an
interaction
that
has
functional
and
pathological
relevance
neuronal
cells
considered
for
underlying
mechanisms
PD.
Transverse
longitudinal
15N
relaxation
revealed
dynamical
properties
αS
bound
outer
membrane
(OMM)
are
different
from
those
cytosolic
state,
thus
indicating
generally
not
interact
fact
affected
by
spatial
proximity
lipid
bilayer.
Moreover,
changes
composition
OMM
dyshomeostasis
PD
were
found
significantly
perturb
topology
state
αS.
Taken
together,
our
data
underline
characterizing
achieve
accurate
understanding
these
elusive
play
numerous
processes
occurring
surfaces.
Язык: Английский