Advance in peptide-based drug development: delivery platforms, therapeutics and vaccines
Signal Transduction and Targeted Therapy,
Год журнала:
2025,
Номер
10(1)
Опубликована: Март 5, 2025
The
successful
approval
of
peptide-based
drugs
can
be
attributed
to
a
collaborative
effort
across
multiple
disciplines.
integration
novel
drug
design
and
synthesis
techniques,
display
library
technology,
delivery
systems,
bioengineering
advancements,
artificial
intelligence
have
significantly
expedited
the
development
groundbreaking
drugs,
effectively
addressing
obstacles
associated
with
their
character,
such
as
rapid
clearance
degradation,
necessitating
subcutaneous
injection
leading
increasing
patient
discomfort,
ultimately
advancing
translational
research
efforts.
Peptides
are
presently
employed
in
management
diagnosis
diverse
array
medical
conditions,
diabetes
mellitus,
weight
loss,
oncology,
rare
diseases,
additionally
garnering
interest
facilitating
targeted
platforms
advancement
vaccines.
This
paper
provides
an
overview
present
market
clinical
trial
progress
therapeutics,
platforms,
It
examines
key
areas
through
literature
analysis
emphasizes
structural
modification
principles
well
recent
advancements
screening,
design,
technologies.
accelerated
including
peptide-drug
complexes,
new
vaccines,
innovative
diagnostic
reagents,
has
potential
promote
era
precise
customization
disease
therapeutic
schedule.
Язык: Английский
Hierarchically Engineered Self-Adaptive Nanoplatform Guided Intuitive and Precision Interventions for Deep-Seated Glioblastoma
ACS Nano,
Год журнала:
2025,
Номер
unknown
Опубликована: Янв. 3, 2025
Glioblastoma
multiforme
(GBM),
particularly
the
deep-seated
tumor
where
surgical
removal
is
not
feasible,
poses
great
challenges
for
clinical
treatments
due
to
complicated
biological
barriers
and
risk
of
damaging
healthy
brain
tissue.
Here,
we
hierarchically
engineer
a
self-adaptive
nanoplatform
(SAN)
that
overcomes
delivery
by
dynamically
adjusting
its
structure,
surface
charge,
particle
size,
targeting
moieties
precisely
distinguish
between
parenchyma
cells.
We
further
devise
Язык: Английский
Nanotherapy of Glioblastoma—Where Hope Grows
International Journal of Molecular Sciences,
Год журнала:
2025,
Номер
26(5), С. 1814 - 1814
Опубликована: Фев. 20, 2025
Localization
in
the
central
nervous
system,
diffuse
growth,
presence
of
stem
cells,
and
numerous
resistance
mechanisms,
all
make
glioblastoma
(GBM)
an
incurable
tumor.
The
standard
treatment
GBM
consisting
surgery;
radio-
chemotherapy
with
temozolomide
provides
insufficient
therapeutic
benefit
needs
to
be
updated
effective
modern
solutions.
One
most
promising
intensively
explored
approaches
against
is
use
nanotherapy.
first,
so
far
only,
nanoparticle-based
therapy
approved
for
NanoThermTM.
It
based
on
iron
oxide
nanoparticles
thermal
ablation
tumor
a
magnetic
field.
Numerous
other
types
nanotherapies
are
being
evaluated,
including
polymer
lipid-based
nanoformulations,
nanodiscs,
dendrimers,
metallic,
silica,
or
bioderived
nanoparticles,
among
others.
advantages
these
nanoscale
drug
carriers
include
improved
penetration
across
blood-brain
barrier,
targeted
delivery,
biocompatibility,
lower
systemic
toxicity,
while
major
problems
their
implementation
involve
scaling
up
production
high
costs.
Nevertheless,
taking
impressive
benefits
into
consideration,
it
seems
obvious
that
combined
effort
scientific
world
will
need
taken
tackle
challenges
implement
novel
therapies
clinics,
giving
hope
battle
can
finally
won.
Язык: Английский
Targeted Delivery of Nanoparticle-Conveyed Neutrophils to the Glioblastoma Site for Efficient Therapy
ACS Applied Materials & Interfaces,
Год журнала:
2024,
Номер
16(32), С. 41819 - 41827
Опубликована: Июль 26, 2024
Glioblastoma
is
a
common
brain
tumor
that
poses
considerable
challenges
in
drug
delivery.
In
this
study,
we
investigated
the
potential
of
cell-based
nanoparticles
for
targeted
delivery
to
glioblastoma
sites.
The
anticancer
temozolomide
(TMZ)-loaded
T7-cholesterol
nanoparticle
micelles
efficiently
delivered
neutrophils
and,
subsequently,
tumors.
T7
cell-penetrating
peptide
enhances
T7/TMZ
target
cells.
also
serves
as
transferrin
peptide,
enabling
T7-conjugated
cholesterol
can
self-assemble
into
aqueous
solution
and
attach
membrane
neutrophils.
We
confirmed
were
located
inside
Thereafter,
T7/TMZ-conveyed
administered
mouse
model,
penetrate
blood-brain
barrier
deliver
drugs
directly
site.
evaluated
efficiency
therapeutic
effects
intravenous
injection
model.
These
results
demonstrate
promising
role
neutrophil-based
systems
therapy
glioblastoma.
Язык: Английский
Recent Progress in the Development of Peptide-Drug Conjugates (PDCs) for Cancer Therapy
European Journal of Medicinal Chemistry,
Год журнала:
2024,
Номер
284, С. 117204 - 117204
Опубликована: Дек. 24, 2024
Язык: Английский
Targeted delivery of SN38 to breast cancer using amphiphilic diblock copolymers PHPMA-b-PBAEM as micellar carriers with AS1411 aptamer
International Journal of Pharmaceutics,
Год журнала:
2024,
Номер
661, С. 124387 - 124387
Опубликована: Июнь 24, 2024
Breast
cancer
treatment
can
be
challenging,
but
a
targeted
drug
delivery
system
(DDS)
has
the
potential
to
make
it
more
effective
and
reduce
side
effects.
This
study
presents
novel
nanotherapeutic
DDS
developed
through
self-assembly
of
an
amphiphilic
di-block
copolymer
deliver
chemotherapy
SN38
specifically
breast
cells.
The
vehicle
was
constructed
from
PHPMA-b-PEAMA
diblock
synthesized
via
RAFT
polymerization.
A
single
emulsion
method
then
used
encapsulate
within
nanoparticles
(NPs)
formed
copolymer.
AS1411
DNA
aptamer
covalently
bonded
surface
micellar
NPs,
producing
DDS.
Molecular
dynamics
(MD)
simulation
studies
were
also
performed
on
di
block
polymeric
system,
demonstrating
that
interacted
well
with
block.
in
vitro
results
demonstrated
AS1411-
decorated
SN38-loaded
HPMA
NPs
highly
toxic
cells
while
having
minimal
effect
non-cancerous
Remarkably,
vivo
elucidated
ability
enhance
antitumor
SN38,
suppressing
tumor
growth
improving
survival
rates
compared
free
SN38.
Язык: Английский
Novel Cyclic Peptide–Drug Conjugate P6-SN38 Toward Targeted Treatment of EGFR Overexpressed Non-Small Cell Lung Cancer
Pharmaceutics,
Год журнала:
2024,
Номер
16(12), С. 1613 - 1613
Опубликована: Дек. 19, 2024
Background/Objectives:
Here,
we
report
on
the
synthesis
and
biological
evaluation
of
a
novel
peptide–drug
conjugate,
P6-SN38,
which
consists
EGFR-specific
short
cyclic
peptide,
P6,
Topo
I
inhibitor
SN38,
is
bioactive
metabolite
anticancer
drug
irinotecan.
Methods:
SN38
attached
to
peptide
at
position
20
E
ring’s
tertiary
hydroxyl
group
via
mono-succinate
linker.
Results:
The
developed
conjugate
(PDC)
exhibited
sub-micromolar
activity
EGFR-positive
(EGFR+)
cell
lines
but
no
effect
EGFR-negative
(EGFR−)
cells.
In
vivo
studies
have
shown
that
this
PDC
specifically
accumulates
in
EGFR+
non-small
lung
cancer
(NSCLC)
xenografts
presents
superior
compared
antibody
cetuximab
(ErbituxTM)
free
SN38.
10
mg/kg
dose
P6-SN38
side-by-side
EGFR+/EGFR−
xenograft
shows
eradication
tumor
with
good
tolerance,
inhibition
growth
EGFR−
counterpart.
Conclusions:
examined
study
was
proven
be
highly
efficient
for
NSCLC,
broadening
its
utilization
targeted
therapy
EGFR
overexpressed
cancers.
Язык: Английский