Small,
Journal Year:
2024,
Volume and Issue:
unknown
Published: Dec. 17, 2024
Extensive
accumulation
of
senescent
cells
contributes
to
organismal
aging,
and
slowing
down
the
process
cellular
senescence
may
ameliorate
age-related
pathologies.
Targeted
inhibition
mechanistic
target
rapamycin
complex
1
(mTORC1)
is
found
suppress
conversion
senescence.
The
regulatory-associated
protein
mTOR
(Raptor),
a
key
component
mTORC1,
has
been
implicated
as
important
in
aging
process,
its
druggability
deserves
be
investigated.
Due
high
efficiency
convenience
drug
construction,
siRNA
shows
great
potential
silencing
Raptor
expression
via
RNA
interfering
therapy.
Here,
we
developed
functionalized
anti-aging
nanoplatform
based
on
tetrahedral
DNA
nanostructures
(TDNs)
encapsulating
targeting
for
synergistic
therapy,
named
siR-TDN
JACS Au,
Journal Year:
2025,
Volume and Issue:
5(2), P. 486 - 520
Published: Feb. 10, 2025
Tetrahedral
framework
nucleic
acids
(tFNAs)
represent
a
promising
advancement
in
acid
nanotechnology
due
to
their
unique
structural
properties,
high
biocompatibility,
and
multifaceted
biomedical
applications.
Constructed
through
one-pot
annealing
method,
four
single-stranded
DNAs
self-assemble
into
stable,
three-dimensional
tetrahedral
nanostructures
with
enhanced
mechanical
robustness
physiological
stability,
resisting
enzymatic
degradation.
Their
ability
permeate
mammalian
cells
without
transfection
agents,
coupled
modifiable
surfaces,
positions
tFNAs
as
versatile
carriers
for
drug
gene
delivery
systems.
The
tFNA-based
platforms
exhibit
superior
therapeutic
efficacy,
including
antioxidative
anti-inflammatory
effects,
alongside
efficient
cellular
uptake
tissue
penetration.
These
features
underpin
role
precision
medicine,
enabling
targeted
of
diverse
agents
such
synthetic
compounds,
peptides,
acids.
Additionally,
demonstrate
significant
potential
regenerative
immune
modulation,
antibacterial
strategies,
oncology.
By
addressing
challenges
translational
integration,
stand
poised
accelerate
the
development
research
clinical
applications,
fostering
novel
therapies
enhancing
outcomes
across
wide
spectrum
diseases.
This
Perspective
thoroughly
details
attributes
applications
critically
evaluates
tFNAs'
potential,
outlining
inherent
implementation
exploring
solutions
these
obstacles.
World Journal of Hepatology,
Journal Year:
2023,
Volume and Issue:
15(6), P. 755 - 774
Published: June 25, 2023
Liver
fibrosis
accompanies
the
progression
of
chronic
liver
diseases
independent
etiologies,
such
as
hepatitis
viral
infection,
alcohol
consumption,
and
metabolic-associated
fatty
disease.
It
is
commonly
associated
with
injury,
inflammation,
cell
death.
characterized
by
abnormal
accumulation
extracellular
matrix
components
that
are
expressed
myofibroblasts
collagens
alpha-smooth
actin
proteins.
Activated
hepatic
stellate
cells
contribute
to
major
population
myofibroblasts.
Many
treatments
for
have
been
investigated
in
clinical
trials,
including
dietary
supplementation
(e.g.,
vitamin
C),
biological
treatment
simtuzumab),
drug
pegbelfermin
natural
herbs),
genetic
regulation
non-coding
RNAs),
transplantation
stem
hematopoietic
cells).
However,
none
these
has
approved
Food
Drug
Administration.
The
efficacy
can
be
evaluated
histological
staining
methods,
imaging
serum
biomarkers,
well
scoring
systems,
fibrosis-4
index,
aspartate
aminotransferase
platelet
ratio,
non-alcoholic
disease
score.
Furthermore,
reverse
slowly
frequently
impossible
advanced
or
cirrhosis.
To
avoid
life-threatening
stage
fibrosis,
anti-fibrotic
treatments,
especially
combined
behavior
prevention,
treatment,
drugs
herb
medicines,
needed.
This
review
summarizes
past
studies
current
future
fibrosis.
ACS Applied Materials & Interfaces,
Journal Year:
2024,
Volume and Issue:
16(26), P. 33192 - 33204
Published: June 17, 2024
The
human
body's
primary
line
of
defense,
the
skin,
is
especially
prone
to
harm.
Although
microRNA
(miRNA)-based
therapies
have
attracted
increasing
attention
for
skin
wound
healing,
their
applications
remain
limited
owing
a
range
issues.
Tetrahedral
framework
DNA
(tFNA),
nanomaterial
possessing
nucleic
acid
characteristics,
exhibits
an
excellent
biocompatibility,
in
addition
anti-inflammatory
and
transdermal
delivery
capabilities,
can
accelerate
healing.
Due
its
potential
exert
synergistic
action
with
therapeutic
miRNA,
tFNA
has
been
considered
ideal
vehicle
miRNA
therapy.
design
synthesis
bioswitchable
system
(BiRDS)
reported,
which
contains
three
miRNAs
as
well
core
maximize
loading
capacity
while
preserving
characteristics
tFNA.
A
high
stability,
permeability
cells
tissues
good
biological
compatibility
are
demonstrated.
By
selectively
inhibiting
heparin-binding
epidermal
growth
factor
(HB-EGF),
BiRDS
inhibit
NF-κB
pathway
simultaneously
controlling
PTEN/Akt
pathway.
As
result,
helps
healing
go
through
inflammation
proliferative
phase.
This
study
demonstrates
advantages
miRNA-based
therapy
provides
new
research
ideas
treatment
skin-related
diseases.
Frontiers in Immunology,
Journal Year:
2023,
Volume and Issue:
14
Published: Dec. 5, 2023
During
fibrosis,
(myo)fibroblasts
deposit
large
amounts
of
extracellular
matrix
proteins,
thereby
replacing
healthy
functional
tissue.
In
liver
this
leads
to
the
loss
hepatocyte
function,
portal
hypertension,
variceal
bleeding,
and
increased
susceptibility
infection.
At
an
early
stage,
fibrosis
is
a
dynamic
reversible
process,
however,
from
cirrhotic
there
significant
progression
hepatocellular
carcinoma.
Both
liver-resident
macrophages
(Kupffer
cells)
monocyte-derived
are
important
drivers
progression,
but
can
also
induce
its
regression
once
triggers
chronic
inflammation
eliminated.
cancer,
they
attracted
tumor
site
become
tumor-associated
(TAMs)
polarized
towards
M2-
anti-inflammatory/tumor-promoting
phenotype.
Besides
their
role
in
thrombosis
hemostasis,
platelets
stimulate
development
by
secreting
profibrogenic
factors
regulating
innate
immune
response,
e.g.,
interacting
with
monocytes
macrophages.
Here,
we
review
recent
literature
on
interplay
Frontiers in Immunology,
Journal Year:
2023,
Volume and Issue:
14
Published: May 30, 2023
Primary
biliary
cholangitis
(PBC)
is
an
immune-mediated
liver
disease
characterized
by
cholestasis,
injuries,
fibrosis,
and
chronic
non-suppurative
cholangitis.
The
pathogenesis
of
PBC
multifactorial
involves
immune
dysregulation,
abnormal
bile
metabolism,
progressive
ultimately
leading
to
cirrhosis
failure.
Ursodeoxycholic
acid
(UDCA)
obeticholic
(OCA)
are
currently
used
as
first-
second-line
treatments,
respectively.
However,
many
patients
do
not
respond
adequately
UDCA,
the
long-term
effects
these
drugs
limited.
Recent
research
has
advanced
our
understanding
mechanisms
in
greatly
facilitated
development
novel
target
mechanistic
checkpoints.
Animal
studies
clinical
trials
pipeline
have
yielded
promising
results
slowing
progression.
Targeting
mediated
anti-inflammatory
therapies
focused
on
early
stage,
while
anti-cholestatic
anti-fibrotic
emphasized
late
stage
disease,
which
fibrosis
development.
Nonetheless,
it
worth
noting
that
currently,
there
exists
a
dearth
therapeutic
options
can
effectively
impede
progression
its
terminal
stages.
Hence,
urgent
need
for
further
aimed
at
investigating
underlying
pathophysiology
with
potential
effects.
This
review
highlights
current
knowledge
immunological
cellular
PBC.
Further,
we
also
address
mechanism-based
strategies
improve
efficacy
existing
treatments.
