Abstract
Aging
is
a
major
risk
factor
for
most
chronic
disorders,
which
cellular
senescence
one
of
the
central
hallmarks.
Senescent
cells
develop
pro‐inflammatory
senescence‐associated
secretory
phenotype
(SASP),
significantly
contributes
to
organismal
aging
and
age‐related
disorders.
Development
senotherapeutics,
an
emerging
class
therapeutic
agents
target
senescent
cells,
allows
effectively
delay
alleviate
pathologies.
Here
we
report
preliminary
outputs
from
screening
natural
medicinal
agent
(NMA)
library
senotherapeutic
candidates
validated
several
with
prominent
potential
as
senomorphics.
Rutin,
phytochemical
constituent
found
in
number
plants,
showed
remarkable
capacity
targeting
by
dampening
expression
full
spectrum
SASP.
Further
analysis
indicated
that
rutin
restrains
acute
stress‐associated
(ASAP)
specifically
interfering
interactions
ATM
HIF1α,
master
regulator
systemic
homeostasis
activated
during
senescence,
TRAF6,
part
key
signaling
axis
supporting
ASAP
development
toward
Conditioned
media
produced
stromal
enhanced
malignant
phenotypes
prostate
cancer
including
vitro
proliferation,
migration,
invasion,
more
importantly,
chemoresistance,
while
remarkably
downregulated
these
gain‐of‐functions.
Although
classic
chemotherapy
reduced
tumor
progression,
treatment
outcome
was
substantially
improved
upon
combination
chemotherapeutic
rutin.
Our
study
provides
proof
concept
senomorphic
agent,
presents
effective
avenue
alleviating
pathologies
cancer.
Alzheimer s & Dementia Translational Research & Clinical Interventions,
Год журнала:
2021,
Номер
7(1)
Опубликована: Янв. 1, 2021
Abstract
Introduction
The
number
of
individuals
worldwide
with
Alzheimer's
disease
(AD)
is
growing
at
a
rapid
rate.
New
treatments
are
urgently
needed.
We
review
the
current
pipeline
drugs
in
clinical
trials
for
treatment
AD.
Methods
interrogated
ClinicalTrials.gov,
federal
registry
to
identify
trials.
Results
There
126
agents
152
assessing
new
therapies
AD:
28
Phase
3
trials,
74
2,
and
24
1.
majority
(82.5%)
target
underlying
biology
AD
intent
modification;
10.3%
putative
cognitive
enhancing
agents;
7.1%
being
developed
reduce
neuropsychiatric
symptoms.
Discussion
This
analysis
shows
that
biological
processes
more
diversified,
biomarkers
regularly
used,
repurposed
explored
determine
their
utility
Nature,
Год журнала:
2023,
Номер
620(7973), С. 374 - 380
Опубликована: Авг. 2, 2023
Low-grade
inflammation
is
a
hallmark
of
old
age
and
central
driver
ageing-associated
impairment
disease1.
Multiple
factors
can
contribute
to
inflammation2;
however,
the
molecular
pathways
that
transduce
aberrant
inflammatory
signalling
their
impact
in
natural
ageing
remain
unclear.
Here
we
show
cGAS-STING
pathway,
which
mediates
immune
sensing
DNA3,
critical
chronic
functional
decline
during
ageing.
Blockade
STING
suppresses
phenotypes
senescent
human
cells
tissues,
attenuates
ageing-related
multiple
peripheral
organs
brain
mice,
leads
an
improvement
tissue
function.
Focusing
on
brain,
reveal
activation
triggers
reactive
microglial
transcriptional
states,
neurodegeneration
cognitive
decline.
Cytosolic
DNA
released
from
perturbed
mitochondria
elicits
cGAS
activity
microglia,
defining
mechanism
by
engaged
brain.
Single-nucleus
RNA-sequencing
analysis
microglia
hippocampi
gain-of-function
mouse
model
demonstrates
engagement
sufficient
direct
states
leading
bystander
cell
inflammation,
neurotoxicity
impaired
memory
capacity.
Our
findings
establish
pathway
as
blockade
potential
strategy
halt
neurodegenerative
processes
age.
Journal of Hematology & Oncology,
Год журнала:
2020,
Номер
13(1)
Опубликована: Ноя. 10, 2020
Immunosenescence
is
a
process
of
immune
dysfunction
that
occurs
with
age
and
includes
remodeling
lymphoid
organs,
leading
to
changes
in
the
function
elderly,
which
closely
related
development
infections,
autoimmune
diseases,
malignant
tumors.
T
cell-output
decline
an
important
feature
immunosenescence
as
well
production
senescence-associated
secretory
phenotype,
increased
glycolysis,
reactive
oxygen
species.
Senescent
cells
exhibit
abnormal
phenotypes,
including
downregulation
CD27,
CD28,
upregulation
CD57,
killer
cell
lectin-like
receptor
subfamily
G,
Tim-3,
Tight,
cytotoxic
T-lymphocyte-associated
protein
4,
are
tightly
The
role
tumors
sophisticated:
many
factors
involved
include
cAMP,
glucose
competition,
oncogenic
stress
tumor
microenvironment,
can
induce
senescence
cells,
macrophages,
natural
dendritic
cells.
Accordingly,
these
senescent
could
also
affect
progression.
In
addition,
effect
on
response
checkpoint
blocking
antibody
therapy
so
far
ambiguous
due
low
participation
elderly
cancer
patients
clinical
trials.
Furthermore,
other
senescence-related
interventions
be
possible
genetic
pharmacological
methods,
mTOR
inhibition,
interleukin-7
recombination,
NAD+
activation.
Overall,
this
review
aims
highlight
characteristics
its
impact
immunotherapy,
especially
future
directions
treatment
through
senescence-focused
strategies.
Signal Transduction and Targeted Therapy,
Год журнала:
2021,
Номер
6(1)
Опубликована: Июнь 28, 2021
Remarkable
progress
in
ageing
research
has
been
achieved
over
the
past
decades.
General
perceptions
and
experimental
evidence
pinpoint
that
decline
of
physical
function
often
initiates
by
cell
senescence
organ
ageing.
Epigenetic
dynamics
immunometabolic
reprogramming
link
to
alterations
cellular
response
intrinsic
extrinsic
stimuli,
representing
current
hotspots
as
they
not
only
(re-)shape
individual
identity,
but
also
involve
fate
decision.
This
review
focuses
on
present
findings
emerging
concepts
epigenetic,
inflammatory,
metabolic
regulations
consequences
process.
Potential
therapeutic
interventions
targeting
regulatory
mechanisms,
using
state-of-the-art
techniques
are
discussed.
Nature Metabolism,
Год журнала:
2021,
Номер
3(12), С. 1706 - 1726
Опубликована: Дек. 6, 2021
Abstract
Ageing-associated
functional
decline
of
organs
and
increased
risk
for
age-related
chronic
pathologies
is
driven
in
part
by
the
accumulation
senescent
cells,
which
develop
senescence-associated
secretory
phenotype
(SASP).
Here
we
show
that
procyanidin
C1
(PCC1),
a
polyphenolic
component
grape
seed
extract
(GSE),
increases
healthspan
lifespan
mice
through
its
action
on
cells.
By
screening
library
natural
products,
find
GSE,
PCC1
as
one
active
components,
have
specific
effects
At
low
concentrations,
appears
to
inhibit
SASP
formation,
whereas
it
selectively
kills
cells
at
higher
possibly
promoting
production
reactive
oxygen
species
mitochondrial
dysfunction.
In
rodent
models,
depletes
treatment-damaged
tumour
microenvironment
enhances
therapeutic
efficacy
when
co-administered
with
chemotherapy.
Intermittent
administration
either
irradiated,
cell-implanted
or
naturally
aged
old
alleviates
physical
dysfunction
prolongs
survival.
We
identify
senotherapeutic
agent
vivo
activity
high
potential
further
development
clinical
intervention
delay,
alleviate
prevent
pathologies.
