A Dual‐Targeting Biomimetic Nanoplatform Integrates SDT/CDT/Gas Therapy to Boost Synergistic Ferroptosis for Orthotopic Hepatocellular Carcinoma Therapy
Advanced Science,
Год журнала:
2025,
Номер
unknown
Опубликована: Янв. 9, 2025
Abstract
The
development
of
efficient
therapeutic
strategies
to
promote
ferroptotic
cell
death
offers
significant
potential
for
hepatocellular
carcinoma
(HCC)
treatment.
Herein,
this
study
presents
an
HCC‐targeted
nanoplatform
that
integrates
bimetallic
FeMoO
4
nanoparticles
with
CO‐releasing
molecules,
and
further
camouflaged
SP94
peptide‐modified
macrophage
membrane
enhanced
ferroptosis‐driven
multi‐modal
therapy
HCC.
Leveraging
the
multi‐enzyme
activities
multivalent
metallic
elements,
not
only
decomposes
H
2
O
generate
oxygen
alleviate
tumor
hypoxia
but
also
depletes
glutathione
inactivate
peroxides
4,
which
amplify
sonodynamic
under
ultrasound
(US)
irradiation.
Meanwhile,
catalyzes
Fenton
reaction
produce
hydroxyl
radicals
chemodynamic
therapy.
Elevated
intracellular
reactive
species
trigger
cascade
release
CO,
leading
lethal
lipid
peroxidation
enhancing
ferroptosis‐mediated
This
demonstrates
robust
anti‐tumor
efficacy
US
irradiation
favorable
biosafety
in
both
subcutaneous
orthotopic
HCC
models,
representing
a
promising
approach
Additionally,
findings
offer
new
insights
into
microenvironment
modulation
optimize
US‐triggered
cancer
Язык: Английский
Mitochondrial alterations and signatures in hepatocellular carcinoma
Cancer and Metastasis Reviews,
Год журнала:
2025,
Номер
44(1)
Опубликована: Фев. 18, 2025
Язык: Английский
Overexpression and clinicopathological significance of zinc finger protein 71 in hepatocellular carcinoma
Kai Qin,
Dandan Xiong,
Zhen Qin
и другие.
World Journal of Hepatology,
Год журнала:
2025,
Номер
17(2)
Опубликована: Фев. 20, 2025
BACKGROUND
Hepatocellular
carcinoma
(HCC)
is
one
of
the
most
prevalent
and
aggressive
forms
liver
cancer,
with
high
morbidity
poor
prognosis
due
to
late
diagnosis
limited
treatment
options.
Despite
advances
in
understanding
its
molecular
mechanisms,
effective
biomarkers
for
early
detection
targeted
therapy
remain
scarce.
Zinc
finger
protein
71
(ZNF71),
a
zinc-finger
protein,
has
been
implicated
various
cancers,
yet
role
HCC
remains
largely
unexplored.
This
gap
knowledge
underscores
need
further
investigation
into
ZNF71
potential
as
diagnostic
or
therapeutic
target
HCC.
AIM
To
explore
expression
levels,
clinical
relevance,
mechanisms
progression
METHODS
The
study
evaluated
235
specimens
13
noncancerous
tissue
samples
using
immunohistochemistry.
High-throughput
datasets
were
employed
assess
differential
association
pathological
features.
impact
on
cell
line
growth
was
examined
through
clustered
regularly
interspaced
short
palindromic
repeat
knockout
screens.
Co-expressed
genes
identified
analyzed
enrichment
LinkedOmics
Sangerbox
3.0,
focusing
significant
correlations
(P
<
0.01,
correlation
coefficient
≥
0.3).
Furthermore,
relationship
between
immune
infiltration
quantified
TIMER2.0.
RESULTS
showed
higher
tissues
vs
non-tumorous
tissues,
statistical
difference
0.05).
Data
from
UALCAN
platform
indicated
increased
levels
across
mid-stage
HCC,
correlating
disease
severity
analysis
presented
standardized
mean
0.55
(95%
confidence
interval
[CI]:
0.34-0.75).
efficiency
mRNA
evaluated,
yielding
an
area
under
curve
0.78
(95%CI:
0.75-0.82),
sensitivity
0.63
0.53-0.72),
specificity
0.82
0.73-0.89).
Diagnostic
likelihood
ratios
positive
at
3.61
2.41-5.41)
negative
0.45
0.36-0.56).
strong
such
ZNF470,
ZNF256,
ZNF285.
Pathway
analyses
highlighted
associations
herpes
simplex
virus
type
1
infection,
cycle,
DNA
replication.
Negative
involved
metabolic
pathways,
peroxisomes,
fatty
acid
degradation.
TIMER2.0
demonstrated
types,
including
CD4+
T
cells,
B
regulatory
monocytes,
macrophages,
myeloid
dendritic
cells.
CONCLUSION
significantly
upregulated
disease’s
stages.
It
appears
promote
involving
cycle
metabolism
associated
infiltration.
These
findings
suggest
that
could
be
novel
diagnosing
treating
Язык: Английский
Triggering Pyroptosis in Cancer
Daniel E. Johnson,
Zhibin Cui
Biomolecules,
Год журнала:
2025,
Номер
15(3), С. 348 - 348
Опубликована: Фев. 28, 2025
Pyroptosis
is
an
inflammatory
programmed
cell
death
recently
identified
as
a
crucial
cellular
process
in
various
diseases,
including
cancers.
Unlike
other
forms
of
death,
canonical
pyroptosis
involves
the
specific
cleavage
gasdermin
by
caspase-1,
resulting
membrane
damage
and
release
pro-inflammatory
cytokines
IL-1β
IL-18.
Initially
observed
innate
immune
cells
responding
to
external
pathogens
or
internal
signals,
pyroptotic
has
now
been
numerous
types.
Recent
studies
have
extensively
explored
different
ways
trigger
solid
tumors,
presenting
promising
avenue
for
cancer
treatment.
This
review
outlines
mechanisms
both
noncanonical
pertinent
primarily
focuses
on
biomolecules
that
can
induce
malignancies.
strategy
aims
not
only
eliminate
but
also
promote
improved
tumor
microenvironment.
Furthermore,
emerging
research
indicates
targeting
pathways
may
improve
effectiveness
existing
treatments,
making
them
more
potent
against
resistant
types,
offering
new
hope
overcoming
treatment
resistance
aggressive
Язык: Английский
Machine learning analysis identified NNMT as a potential therapeutic target for hepatocellular carcinoma based on PCD-related genes
Scientific Reports,
Год журнала:
2025,
Номер
15(1)
Опубликована: Март 3, 2025
Язык: Английский
Inflammation and cancer: molecular mechanisms and clinical consequences
Frontiers in Oncology,
Год журнала:
2025,
Номер
15
Опубликована: Март 17, 2025
Inflammation,
a
hallmark
of
cancer,
has
been
associated
with
tumor
progression,
transition
into
malignant
phenotype
and
efficacy
anticancer
treatments
in
cancer.
It
affects
all
stages
from
the
initiation
carcinogenesis
to
metastasis.
Chronic
inflammation
induces
immunosup-pression,
providing
an
environment
conducive
carcinogenesis,
whereas
acute
antitumor
immune
response,
leading
suppression.
Solid
tumors
have
inflammatory
microenvironment
(TME)
containing
cancer
cells,
stromal
soluble
molecules,
which
plays
key
role
progression
therapy
response.
Both
cells
TME
are
highly
plastic
constantly
change
their
phenotypic
functional
properties.
Cancer-associated
inflammation,
majority
consists
innate
important
cell
plasticity,
development
drug
resistance.
Today,
combined
used
advanced
technologies,
such
as
single-cell
RNA
sequencing
spatial
molecular
imaging
analysis,
pathways
linking
chronic
largely
elucidated.
In
this
review
article,
we
highlighted
cellular
mechanisms
involved
cancer-associated
its
effects
on
treatment
We
also
comprehensively
setting
GI
cancers.
Язык: Английский
Mixed lineage kinase domain-like protein in liver diseases: Cell-type-specific functions and dual roles
World Journal of Gastroenterology,
Год журнала:
2025,
Номер
31(14)
Опубликована: Апрель 9, 2025
In
this
letter,
we
comment
on
the
article
by
Xuan
Yuan
et
al,
published
in
recent
issue
of
World
Journal
Gastroenterology.
Mixed
lineage
kinase
domain-like
protein
(MLKL)
exhibits
cell-type-specific
functions
liver
parenchymal
and
non-parenchymal
cells,
playing
dual
roles
pathogenesis
diseases.
hepatocytes,
MLKL
primarily
mediates
necroptosis
inhibits
autophagy,
thereby
exacerbating
injury.
Conversely,
modulates
inflammatory
responses
promotes
fibrotic
processes,
driving
disease
progression.
Notably,
also
demonstrates
protective
under
specific
conditions.
For
instance,
can
inhibit
intracellular
bacterial
replication,
promote
endosomal
trafficking,
facilitate
generation
release
extracellular
vesicles,
potentially
exerting
hepatoprotective
effects.
Understanding
these
mechanisms
action,
including
its
promoting
injury
providing
protection,
is
crucial
for
elucidating
complex
diseases
developing
targeted
therapeutic
strategies.
Язык: Английский
Analysis and identification of PTBP2 as an oncogene in hepatocellular carcinoma
Discover Oncology,
Год журнала:
2025,
Номер
16(1)
Опубликована: Апрель 12, 2025
Язык: Английский
Effects of SARS-CoV-2 Spike S1 Subunit on the Interplay Between Hepatitis B and Hepatocellular Carcinoma Related Molecular Processes in Human Liver
Livers,
Год журнала:
2024,
Номер
5(1), С. 1 - 1
Опубликована: Дек. 31, 2024
Background:
This
study
addresses
a
particular
aspect
of
the
biological
behavior
Spike
subunit
S1
SARS-CoV-2.
Researchers
observed
acting
freely
in
human
organism
during
and
after
COVID-19
vaccination.
One
its
properties
is
that
it
interacts
one-to-one
with
proteins.
12
specific
proteins
liver.
Methods:
We
used
these
as
seeds
to
extract
their
functional
relationships
from
proteome
through
enrichment.
The
interactome
representing
set
metabolic
activities
which
they
are
involved
shows
several
molecular
processes
(KEGG),
including
some
linked
HBV
(hepatitis
B)
HCC
(hepatocellular
carcinoma)
many
genes/proteins
involved.
Reports
show
that,
COVID
patients,
reactivated
or
progressed
cancer.
Results:
analyzed
approaches
understand
whether
two
pathologies
have
independent
progressions
common
progression.
All
our
efforts
consistently
showed
involving
both
significantly
present
all
we
used,
making
difficult
any
useful
information
about
fate.
Through
BioGRID,
extracted
experimental
data
vivo
but
derived
model
cell
systems.
lack
patient
STRING
results
prevents
diagnosis
prediction
real
disease
progression;
therefore,
can
consider
them
“aseptic”
data.
Conclusion:
tells
us
genes
HVB-related
pathways
potential
activate
processes.
gold
standard.
It
comparison
similar
interactions
found
individual
phenotypes
phenotype
favors
hinders
also
suggests
how
use
features.
These
sets
constitute
“toolkit”.
In
fact,
if
compare
patient,
will
provide
on
level
phenotypic
state
driving
disease.
composition
an
entire
group
broader
more
detailed
than
single
marker.
Therefore,
protein
compositions
serve
reference
system
doctors
cases
for
personalized
medicine
diagnoses.
Язык: Английский