EBioMedicine,
Год журнала:
2024,
Номер
103, С. 105098 - 105098
Опубликована: Апрель 11, 2024
BackgroundThe
widespread
involvement
of
tumor-infiltrating
B
cells
highlights
their
potential
role
in
tumor
behavior.
However,
cell
heterogeneity
PDAC
remains
unexplored.
Studying
TIL-Bs
aims
to
identify
new
treatment
strategies.MethodsWe
performed
single-cell
RNA
sequencing
study
the
PDAC.
The
prognostic
and
immunologic
value
identified
CD38+
was
explored
FUSCC
(n
=
147)
TCGA
176)
cohorts.
Flow
cytometry
conducted
characterize
relationship
between
other
immune
cells,
as
well
phenotypic
features.
In
vitro
vivo
experiments
were
assess
putative
effect
on
antitumor
immunity.FindingsThe
presence
associated
with
unfavorable
clinicopathological
features
poorer
overall
survival
(p
<
0.001).
Increased
infiltration
accompanied
by
reduced
natural
killer
(NK)
0.021)
increased
regulatory
T
0.016).
Molecular
profiling
revealed
high
expression
IL-10,
IL-35,
TGF-β,
GZMB,
TIM-1,
CD5
CD21,
confirming
cell-like
Co-culture
demonstrated
suppression
NK
cytotoxicity
cell-derived
IL-10
Finally,
suggested
adoptive
transfer
immunity
administration
a
CD38
inhibitor
hampered
growth
0.001).InterpretationWe
discovered
an
independent
factor
use
may
provide
possibilities
for
immunotherapy.FundingThis
supported
National
Natural
Science
Foundation
China
(U21A20374),
Shanghai
Municipal
Technology
Major
Project
(21JC1401500),
Scientific
Innovation
Education
Committee
(2019-01-07-00-07-E00057),
Special
Clinical
Research
Health
Industry
Commission
(No.
20204Y0265)
(23ZR1479300).
Cell Death and Disease,
Год журнала:
2024,
Номер
15(4)
Опубликована: Апрель 4, 2024
Abstract
The
immunosuppressive
microenvironment
caused
by
several
intrinsic
and
extrinsic
mechanism
has
brought
great
challenges
to
the
immunotherapy
of
pancreatic
cancer.
We
identified
GFPT2,
key
enzyme
in
hexosamine
biosynthesis
pathway
(HBP),
as
an
immune-related
prognostic
gene
cancer
using
transcriptome
sequencing
further
confirmed
that
GFPT2
promoted
macrophage
M2
polarization
malignant
phenotype
HBP
is
a
glucose
metabolism
leading
generation
uridine
diphosphate
N-acetylglucosamine
(UDP-GlcNAc),
which
utilized
for
protein
O-GlcNAcylation.
GFPT2-mediated
O-GlcNAcylation
played
important
role
regulating
immune
microenvironment.
Through
cellular
proteomics,
we
IL-18
downstream
CO-IP
mass
spectrum,
YBX1
was
O-GlcNAcylated
nuclear
translocated
Then,
functioned
transcription
factor
promote
transcription.
Our
study
elucidated
relationship
between
metabolic
cells
microenvironment,
might
provide
some
insights
into
combination
therapy
vulnerability
The
occurrence
and
progression
of
tumors
are
often
accompanied
by
disruptions
in
the
gut
microbiota.
Inversely,
impact
microbiota
on
initiation
cancer
is
becoming
increasingly
evident,
influencing
tumor
microenvironment
(TME)
for
both
local
distant
tumors.
Moreover,
it
even
suggested
to
play
a
significant
role
process
immunotherapy,
contributing
high
specificity
therapeutic
outcomes
long-term
effectiveness
across
various
types.
Probiotics,
with
their
generally
positive
influence
microbiota,
may
serve
as
effective
agents
synergizing
immunotherapy.
They
crucial
activating
immune
system
inhibit
growth.
In
summary,
this
comprehensive
review
aims
provide
valuable
insights
into
dynamic
interactions
between
probiotics,
cancer.
Furthermore,
we
highlight
recent
advances
mechanisms
using
probiotics
improve
By
understanding
these
complex
relationships,
unlock
innovative
approaches
diagnosis
treatment
while
optimizing
effects
Pharmaceutics,
Год журнала:
2024,
Номер
16(2), С. 177 - 177
Опубликована: Янв. 26, 2024
Curcumin
is
a
natural
compound
that
has
been
widely
investigated
thanks
to
its
various
biological
properties,
including
antiproliferative.
This
molecule
acts
on
different
cancers
such
as
lung,
breast,
pancreatic,
colorectal,
etc.
However,
the
bioactive
actions
of
curcumin
have
limitations
when
physicochemical
properties
compromise
pharmacological
potential.
As
therapeutic
strategy
against
cancer,
associated
with
inorganic
nanoparticles.
These
nanocarriers
are
capable
delivering
and
offering
synergistically
enhance
anticancer
properties.
review
highlights
types
curcumin-based
nanoparticles
discusses
their
in
vivo
activity
models
cancer.
Cell Death Discovery,
Год журнала:
2024,
Номер
10(1)
Опубликована: Фев. 24, 2024
Abstract
Pancreatic
ductal
adenocarcinoma
(PDAC)
is
a
kind
of
tumor
lacking
nutrients
due
to
its
poor
vascularity
and
desmoplasia.
Recent
studies
have
shown
that
cancer
cells
might
achieve
growth
advantage
through
epitranscriptome
reprogramming.
However,
the
role
m
5
C
in
PDAC
was
not
fully
understood.
We
found
Aly/REF
export
factor
(ALYREF),
reader
modification,
overexpressed
PDAC,
associated
with
bad
prognosis.
In
addition,
ALYREF
expression
negatively
related
CD8
+
T
infiltration
clinical
samples.
knockdown
decreased
vivo
partly
dependent
immunity.
silencing
SLC7A5
subsequently
inactivated
mTORC1
pathway,
resulting
proliferation.
Mechanically,
specifically
recognized
sites
JunD
mRNA,
maintained
stabilization
mRNA
upregulated
transcription
SLC7A5.
Since
key
transporter
large
neutral
amino
acids
(LNAAs),
overexpression
on
depleted
acid
microenvironment
restricted
function.
Moreover,
ALYREF-JunD-SLC7A5
axis
survival
TMA
assays.
conclusion,
this
research
revealed
relationship
between
transportation
immune
microenvironment.
be
novel
target
for
metabolic
vulnerability
surveillance.
EBioMedicine,
Год журнала:
2024,
Номер
103, С. 105098 - 105098
Опубликована: Апрель 11, 2024
BackgroundThe
widespread
involvement
of
tumor-infiltrating
B
cells
highlights
their
potential
role
in
tumor
behavior.
However,
cell
heterogeneity
PDAC
remains
unexplored.
Studying
TIL-Bs
aims
to
identify
new
treatment
strategies.MethodsWe
performed
single-cell
RNA
sequencing
study
the
PDAC.
The
prognostic
and
immunologic
value
identified
CD38+
was
explored
FUSCC
(n
=
147)
TCGA
176)
cohorts.
Flow
cytometry
conducted
characterize
relationship
between
other
immune
cells,
as
well
phenotypic
features.
In
vitro
vivo
experiments
were
assess
putative
effect
on
antitumor
immunity.FindingsThe
presence
associated
with
unfavorable
clinicopathological
features
poorer
overall
survival
(p
<
0.001).
Increased
infiltration
accompanied
by
reduced
natural
killer
(NK)
0.021)
increased
regulatory
T
0.016).
Molecular
profiling
revealed
high
expression
IL-10,
IL-35,
TGF-β,
GZMB,
TIM-1,
CD5
CD21,
confirming
cell-like
Co-culture
demonstrated
suppression
NK
cytotoxicity
cell-derived
IL-10
Finally,
suggested
adoptive
transfer
immunity
administration
a
CD38
inhibitor
hampered
growth
0.001).InterpretationWe
discovered
an
independent
factor
use
may
provide
possibilities
for
immunotherapy.FundingThis
supported
National
Natural
Science
Foundation
China
(U21A20374),
Shanghai
Municipal
Technology
Major
Project
(21JC1401500),
Scientific
Innovation
Education
Committee
(2019-01-07-00-07-E00057),
Special
Clinical
Research
Health
Industry
Commission
(No.
20204Y0265)
(23ZR1479300).
