Journal of Clinical Medicine,
Год журнала:
2024,
Номер
13(11), С. 3098 - 3098
Опубликована: Май 25, 2024
Alzheimer's
disease
(AD)
causes
a
significant
challenge
to
global
healthcare
systems,
with
limited
effective
treatments
available.
This
review
examines
the
landscape
of
novel
therapeutic
strategies
for
AD,
focusing
on
shortcomings
traditional
therapies
against
amyloid-beta
(Aβ)
and
exploring
emerging
alternatives.
Despite
decades
research
emphasizing
role
Aβ
accumulation
in
AD
pathogenesis,
clinical
trials
targeting
have
obtained
disappointing
results,
highlighting
complexity
pathophysiology
need
investigating
other
approaches.
In
this
manuscript,
we
first
discuss
challenges
associated
anti-Aβ
therapies,
including
efficacy
potential
adverse
effects,
underscoring
necessity
alternative
mechanisms
targets.
Thereafter,
promising
non-Aβ-based
strategies,
such
as
tau-targeted
neuroinflammation
modulation,
gene
stem
cell
therapy.
These
approaches
offer
new
avenues
treatment
by
addressing
additional
pathological
hallmarks
downstream
effects
beyond
deposition.
Signal Transduction and Targeted Therapy,
Год журнала:
2024,
Номер
9(1)
Опубликована: Авг. 23, 2024
Abstract
Alzheimer’s
disease
(AD)
stands
as
the
predominant
form
of
dementia,
presenting
significant
and
escalating
global
challenges.
Its
etiology
is
intricate
diverse,
stemming
from
a
combination
factors
such
aging,
genetics,
environment.
Our
current
understanding
AD
pathologies
involves
various
hypotheses,
cholinergic,
amyloid,
tau
protein,
inflammatory,
oxidative
stress,
metal
ion,
glutamate
excitotoxicity,
microbiota-gut-brain
axis,
abnormal
autophagy.
Nonetheless,
unraveling
interplay
among
these
pathological
aspects
pinpointing
primary
initiators
require
further
elucidation
validation.
In
past
decades,
most
clinical
drugs
have
been
discontinued
due
to
limited
effectiveness
or
adverse
effects.
Presently,
available
primarily
offer
symptomatic
relief
often
accompanied
by
undesirable
side
However,
recent
approvals
aducanumab
(
1
)
lecanemab
2
Food
Drug
Administration
(FDA)
present
potential
in
disrease-modifying
Nevertheless,
long-term
efficacy
safety
need
Consequently,
quest
for
safer
more
effective
persists
formidable
pressing
task.
This
review
discusses
pathogenesis,
advances
diagnostic
biomarkers,
latest
updates
trials,
emerging
technologies
drug
development.
We
highlight
progress
discovery
selective
inhibitors,
dual-target
allosteric
modulators,
covalent
proteolysis-targeting
chimeras
(PROTACs),
protein-protein
interaction
(PPI)
modulators.
goal
provide
insights
into
prospective
development
application
novel
drugs.
Cell Reports,
Год журнала:
2024,
Номер
43(2), С. 113761 - 113761
Опубликована: Фев. 1, 2024
Mutations
that
cause
familial
Alzheimer's
disease
(FAD)
are
found
in
amyloid
precursor
protein
(APP)
and
presenilin,
the
catalytic
component
of
γ-secretase,
together
produce
β-peptide
(Aβ).
Nevertheless,
whether
Aβ
is
primary
driver
remains
controversial.
We
report
here
FAD
mutations
disrupt
initial
proteolytic
events
multistep
processing
APP
substrate
C99
by
γ-secretase.
Cryoelectron
microscopy
reveals
a
mimetic
traps
γ-secretase
during
transition
state,
this
structure
aligns
with
activated
enzyme-substrate
complex
captured
molecular
dynamics
simulations.
In
silico
simulations
cellulo
fluorescence
support
stabilization
complexes
mutations.
Neuronal
expression
and/or
presenilin-1
Caenorhabditis
elegans
leads
to
synaptic
loss
only
FAD-mutant
transgenes.
Designed
stabilize
block
production
likewise
led
loss.
Collectively,
these
findings
implicate
stalled
process—not
products—of
cleavage
substrates
pathogenesis.
International Journal of Molecular Sciences,
Год журнала:
2023,
Номер
24(19), С. 14499 - 14499
Опубликована: Сен. 24, 2023
Over
the
past
30
years,
majority
of
(pre)clinical
efforts
to
find
an
effective
therapy
for
Alzheimer’s
disease
(AD)
focused
on
clearing
β-amyloid
peptide
(Aβ)
from
brain
since,
according
amyloid
cascade
hypothesis,
was
(and
it
is
still
considered
by
many)
pathogenic
determinant
this
neurodegenerative
disorder.
However,
as
reviewed
in
article,
results
numerous
clinical
trials
that
have
tested
anti-Aβ
therapies
date
indicate
plays
a
minor
role
pathogenesis
AD.
Indeed,
even
Aducanumab
and
Lecanemab,
two
antibodies
recently
approved
FDA
AD
therapy,
well
Donanemab
showed
limited
efficacy
cognitive
parameters
phase
III
trials,
despite
their
capability
markedly
lowering
Aβ
load.
Furthermore,
preclinical
evidence
demonstrates
possesses
several
physiological
functions,
including
memory
formation,
suggesting
may
part
be
due
loss
function
peptide.
Finally,
generally
accepted
could
result
many
molecular
dysfunctions,
therefore,
if
we
keep
chasing
only
Aβ,
means
cannot
see
forest
trees.
This
review
analyzes
the
role
of
TNF-α
and
its
increase
in
biological
fluids
mild
cognitive
impairment,
Alzheimer’s
disease
(AD).
The
potential
inhibition
with
pharmacological
strategies
paves
way
for
preventing
AD
improving
function
people
at
risk
dementia.
We
conducted
a
narrative
to
characterize
evidence
relation
involvement
possible
therapeutic
inhibition.
Several
studies
report
that
patients
RA
systemic
inflammatory
diseases
treated
blocking
agents
reduce
probability
emerging
dementia
compared
general
population.
Animal
model
also
showed
interesting
results
are
discussed.
An
increasing
amount
basic
scientific
data
clinical
underscore
importance
processes
subsequent
glial
activation
pathogenesis
AD.
targeted
therapy
is
biologically
plausible
approach
cognition
preservation
further
trials
necessary
investigate
benefits
populations
developing
International Journal of Molecular Sciences,
Год журнала:
2024,
Номер
25(7), С. 3892 - 3892
Опубликована: Март 31, 2024
The
amyloid
cascade
hypothesis
for
Alzheimer's
disease
is
still
alive,
although
heavily
challenged.
Effective
anti-amyloid
immunotherapy
would
confirm
the
hypothesis'
claim
that
protein
amyloid-beta
cause
of
disease.
Two
antibodies,
aducanumab
and
lecanemab,
have
been
approved
by
U.S.
Food
Drug
Administration,
while
a
third,
donanemab,
under
review.
main
argument
FDA
approvals
presumed
therapy-induced
removal
cerebral
deposits.
Lecanemab
donanemab
are
also
thought
to
some
statistical
delay
in
determination
cognitive
decline.
However,
clinical
efficacy
less
than
with
conventional
treatment,
selection
amyloid-positive
trial
patients
non-specific
amyloid-PET
imaging,
uncertain
amyloids
trials
cast
doubt
on
this
anti-Alzheimer's
antibody
therapy
hence
hypothesis,
calling
more
thorough
investigation
negative
impact
type
brain.
Journal of Clinical Medicine,
Год журнала:
2024,
Номер
13(2), С. 536 - 536
Опубликована: Янв. 17, 2024
Background:
The
concept
of
Alzheimer
disease
(AD)—since
its
histological
discovery
by
to
the
present
day—has
undergone
substantial
modifications.
Methods:
We
conducted
a
classical
narrative
review
this
field
with
bibliography
selection
(giving
preference
Medline
best
match).
Results:
following
subjects
are
reviewed
and
discussed:
Alzheimer’s
discovery,
Kraepelin’s
creation
new
that
was
rare
condition
until
1970′s,
growing
interest
investment
in
AD
as
major
killer
society
large
elderly
population
second
half
20th
century,
consolidation
clinicopathological
model,
modern
nosology
based
on
dominant
amyloid
hypothesis
among
many
others.
In
21st
development
biomarkers
has
supported
novel
biological
definition
AD,
although
proposed
therapies
have
failed
cure
disease.
incidence
dementia/AD
shown
decrease
affluent
countries
(possibly
due
control
risk
factors),
mixed
dementia
been
established
most
frequent
etiology
oldest
old.
Conclusions:
current
lacks
unanimity.
Many
hypotheses
attempt
explain
complex
physiopathology
entwined
aging,
cascade
yielded
poor
therapeutic
results.
reduction
appears
promising
but
it
should
be
confirmed
future.
A
reevaluation
is
also
necessary.
International Journal of Molecular Sciences,
Год журнала:
2024,
Номер
25(8), С. 4323 - 4323
Опубликована: Апрель 13, 2024
Neurodegenerative
disorders
(NDs)
represent
a
group
of
different
diseases
characterized
by
the
progressive
degeneration
and
death
nervous
system's
cells.
The
diagnosis
is
challenging,
especially
in
early
stages,
due
to
no
specific
clinical
signs
symptoms.
In
this
context,
laboratory
medicine
could
support
clinicians
detecting
differentiating
NDs.
Indeed,
biomarkers
indicate
pathological
mechanisms
underpinning
ideal
biofluid
for
NDs
cerebrospinal
fluid
(CSF),
which
has
limitations,
hampering
its
widespread
use
practice.
However,
intensive
efforts
are
underway
introduce
high-sensitivity
analytical
methods
detect
ND
alternative
nonivasive
biofluid,
such
as
blood
or
saliva.
This
study
presents
an
overview
molecular
currently
used
For
some
diseases,
Alzheimer's
disease
multiple
sclerosis,
well
established
recommended
guidelines.
most
NDs,
research
ongoing
identify
reliable
biomarkers,
consensus
yet
been
achieved.
