MedComm,
Journal Year:
2024,
Volume and Issue:
5(10)
Published: Oct. 1, 2024
Abstract
Glycoproteins,
representing
a
significant
proportion
of
posttranslational
products,
play
pivotal
roles
in
various
biological
processes,
such
as
signal
transduction
and
immune
response.
Abnormal
glycosylation
may
lead
to
structural
functional
changes
glycoprotein,
which
is
closely
related
the
occurrence
development
diseases.
Consequently,
exploring
protein
can
shed
light
on
mechanisms
behind
disease
manifestation
pave
way
for
innovative
diagnostic
therapeutic
strategies.
Nonetheless,
study
clinical
glycoproteomics
fraught
with
challenges
due
low
abundance
intricate
structures
glycosylation.
Recent
advancements
mass
spectrometry‐based
have
improved
our
ability
identify
abnormal
glycoproteins
samples.
In
this
review,
we
aim
provide
comprehensive
overview
foundational
principles
recent
glycoproteomic
methodologies
applications.
Furthermore,
discussed
typical
characteristics,
underlying
functions,
diseases,
brain
cardiovascular
cancers,
kidney
metabolic
Additionally,
highlighted
potential
avenues
future
glycoproteomics.
These
insights
provided
review
will
enhance
comprehension
methods
diseases
promote
elucidation
pathogenesis
discovery
novel
biomarkers
targets.
Journal of Experimental & Clinical Cancer Research,
Journal Year:
2023,
Volume and Issue:
42(1)
Published: June 16, 2023
Abstract
AXL
is
a
member
of
the
TAM
(TYRO3,
AXL,
and
MERTK)
receptor
tyrosine
kinases
family
(RTKs),
its
abnormal
expression
has
been
linked
to
clinicopathological
features
poor
prognosis
cancer
patients.
There
mounting
evidence
supporting
AXL's
role
in
occurrence
progression
cancer,
as
well
drug
resistance
treatment
tolerance.
Recent
studies
revealed
that
reducing
can
weaken
cells'
resistance,
indicating
may
be
promising
target
for
anti-cancer
treatment.
This
review
aims
summarize
structure,
mechanisms
regulating
activating
it,
pattern,
especially
drug-resistant
cancers.
Additionally,
we
will
discuss
diverse
functions
mediating
potential
inhibitors
Signal Transduction and Targeted Therapy,
Journal Year:
2025,
Volume and Issue:
10(1)
Published: Feb. 9, 2025
Abstract
AXL,
a
member
of
the
TAM
receptor
family,
has
emerged
as
potential
target
for
advanced-stage
human
malignancies.
It
is
frequently
overexpressed
in
different
cancers
and
plays
significant
role
various
tumor-promoting
pathways,
including
cancer
cell
proliferation,
invasion,
metastasis,
epithelial–mesenchymal
transition
(EMT),
angiogenesis,
stemness,
DNA
damage
response,
acquired
therapeutic
resistance,
immunosuppression,
inflammatory
responses.
Beyond
oncology,
AXL
also
facilitates
viral
infections,
SARS-CoV-2
Zika
highlighting
its
importance
both
virology.
In
preclinical
models,
small-molecule
kinase
inhibitors
targeting
have
shown
promising
anti-tumorigenic
potential.
This
review
primarily
focuses
on
induction,
regulation
biological
functions
mediating
these
pathways.
We
discuss
range
strategies,
recently
developed
tyrosine
(TKIs),
monoclonal
antibodies,
antibody–drug
conjugates
(ADCs),
anti-AXL-CAR,
combination
therapies.
These
interventions
are
being
examined
clinical
studies,
offering
improved
drug
sensitivity
efficacy.
further
mechanisms
particularly
crosstalk
between
other
critical
kinases
(RTKs)
such
c-MET,
EGFR,
HER2/HER3,
VEGFR,
PDGFR,
FLT3.
Finally,
we
highlight
key
research
areas
that
require
exploration
to
enhance
AXL-mediated
approaches
outcomes.
Journal of Hematology & Oncology,
Journal Year:
2023,
Volume and Issue:
16(1)
Published: Jan. 24, 2023
Abstract
Despite
significant
progress
in
clinical
management,
drug
resistance
remains
a
major
obstacle.
Recent
research
based
on
protein
degradation
to
restrain
has
attracted
wide
attention,
and
several
therapeutic
strategies
such
as
inhibition
of
proteasome
with
bortezomib
proteolysis-targeting
chimeric
have
been
developed.
Compared
intervention
at
the
transcriptional
level,
targeting
process
seems
be
more
rapid
direct
strategy.
Proteasomal
proteolysis
lysosomal
are
most
critical
quality
control
systems
responsible
for
proteins
or
organelles.
Although
proteasomal
inhibitors
(e.g.,
chloroquine)
achieved
certain
improvements
some
application
scenarios,
their
routine
practice
is
still
long
way
off,
which
due
lack
precise
capabilities
inevitable
side
effects.
In-depth
studies
regulatory
mechanism
regulators,
including
E3
ubiquitin
ligases,
deubiquitylating
enzymes
(DUBs),
chaperones,
expected
provide
clues
developing
reducing
Here,
we
discuss
underlying
mechanisms
regulating
efflux,
metabolism,
DNA
repair,
target
alteration,
downstream
bypass
signaling,
sustaining
stemness,
tumor
microenvironment
remodeling
delineate
functional
roles
resistance.
We
also
highlight
specific
DUBs,
discussing
possible
modulating
cancer
A
systematic
summary
molecular
basis
by
regulates
will
help
facilitate
development
appropriate
strategies.
International Journal of Nanomedicine,
Journal Year:
2024,
Volume and Issue:
Volume 19, P. 1509 - 1538
Published: Feb. 1, 2024
Abstract:
Lungs
experience
frequent
interactions
with
the
external
environment
and
have
an
abundant
supply
of
blood;
therefore,
they
are
susceptible
to
invasion
by
pathogenic
microorganisms
tumor
cells.
However,
limited
pharmacokinetics
conventional
drugs
in
lungs
poses
a
clinical
challenge.
The
emergence
different
nano-formulations
has
been
facilitated
advancements
nanotechnology.
Inhaled
nanomedicines
exhibit
better
targeting
prolonged
therapeutic
effects.
Although
great
potential,
still
present
several
unknown
risks.
Herein,
we
review
(1)
physiological
anatomy
their
biological
barriers,
(2)
toxicology
nanomaterial
formulations
lungs;
(3)
current
nanomaterials
that
can
be
applied
respiratory
system
related
design
strategies,
(4)
applications
inhaled
treating
disorders,
vaccine
design,
imaging
detection
based
on
characteristics
nanomaterials.
Finally,
(5)
analyze
summarize
challenges
prospects
for
disease
applications.
We
believe
nanomaterials,
particularly
nano-formulations,
excellent
application
diseases.
emphasize
simultaneous
toxic
side
effects
must
considered
during
these
emerging
medicines.
This
study
aims
offer
comprehensive
guidelines
valuable
insights
conducting
research
domain
system.
Keywords:
nanoparticles,
system,
lungs,
nanotechnology
Discover Oncology,
Journal Year:
2025,
Volume and Issue:
16(1)
Published: Feb. 15, 2025
Almonertinib
is
a
third-generation
EGFR-TKI,
and
studies
on
its
resistance
mechanisms
are
lacking.
Cancer-associated
fibroblasts
(CAFs)
can
influence
to
targeted
therapeutics,
but
their
role
mechanism
of
action
in
relation
almonertinib
unclear.
The
study
explored
relationships
among
glycolysis,
cancer-associated
(CAFs),
resistance.
A
dose-escalation
method
was
used
develop
the
almonertinib-resistant
cell
line
H1975AR.
Hexokinase
2
(HK2)
effects
were
evaluated
using
Cell
Counting
Kit-8
assays,
transcriptome
sequencing,
western
blotting,
real-time
PCR,
siRNA
glucose
consumption,
lactate
production
assays.
Differential
gene
expression
analysis
assays
H1975
cells
cultured
with
CAF-conditioned
medium
(H1975/CAF-CM)
revealed
S-phase
kinase-associated
protein
(SKP2)
as
target
driving
HK2.
impact
HK2
inhibitors
H1975/CAF-CM
assessed
colony
formation,
wound
healing,
transwell,
flow
cytometry
apoptosis
H1975AR
displayed
elevated
glycolysis
Subsequently,
we
showed
that
knockdown
reduced
cells.
induced
upregulation
HK2,
which
reversed
by
SKP2.
CAFs
regulate
HK2-mediated
through
SKP2,
promoting
NSCLC.
promotes
Cancers,
Journal Year:
2022,
Volume and Issue:
14(18), P. 4499 - 4499
Published: Sept. 16, 2022
Mutant
p53
is
one
of
the
most
attractive
targets
for
new
anti-cancer
drugs.
Although
traditionally
regarded
as
difficult
to
drug,
several
strategies
have
recently
become
available
targeting
mutant
protein.
One
promising
these
involves
use
low
molecular
weight
compounds
that
promote
refolding
and
reactivation
its
wild-type
form.
Several
such
reactivating
drugs
are
currently
undergoing
evaluation
in
clinical
trials,
including
eprenetapopt
(APR-246),
COTI-2,
arsenic
trioxide
PC14586.
Of
these,
clinically
advanced
which
has
completed
phase
I,
II
III
latter
patients
with
TP53
myelodysplastic
syndrome.
no
data
on
efficacy
eprenetapopt,
preliminary
results
suggest
drug
relatively
well
tolerated.
Other
progressed
trials
involve
promoting
degradation
protein
exploiting
development
vaccines.
With
all
ongoing
we
should
soon
know
if
can
be
used
cancer
treatment.
If
any
show
efficacy,
it
may
a
transformative
treatment
since
so
prevalent
this
disease.
