Nature Communications,
Год журнала:
2020,
Номер
11(1)
Опубликована: Авг. 18, 2020
Abstract
We
evaluate
gene
editing
of
HSV
in
a
well-established
mouse
model,
using
adeno-associated
virus
(AAV)-delivered
meganucleases,
as
potentially
curative
approach
to
treat
latent
infection.
Here
we
show
that
AAV-delivered
but
not
CRISPR/Cas9,
mediate
highly
efficient
HSV,
eliminating
over
90%
from
superior
cervical
ganglia.
Single-cell
RNA
sequencing
demonstrates
both
and
individual
AAV
serotypes
are
non-randomly
distributed
among
neuronal
subsets
ganglia,
implying
improved
delivery
all
may
lead
even
more
complete
elimination
HSV.
As
predicted,
meganucleases
triple
serotype
combination
results
the
greatest
decrease
ganglionic
loads.
The
levels
observed
these
studies,
if
translated
humans,
would
likely
significantly
reduce
reactivation,
shedding,
lesions.
Further
optimization
meganuclease
activity
is
possible,
offer
pathway
cure
for
Cell Host & Microbe,
Год журнала:
2020,
Номер
27(4), С. 519 - 530
Опубликована: Апрель 1, 2020
Antiretroviral
therapy
(ART)
inhibits
HIV
replication
but
is
not
curative.
During
ART,
the
integrated
genome
persists
indefinitely
within
CD4+
T
cells
and
perhaps
other
cells.
Here,
we
describe
mechanisms
thought
to
contribute
its
persistence
during
treatment
highlight
findings
from
numerous
recent
studies
describing
importance
of
cell
proliferation
in
that
process.
Continued
progress
elucidating
biology
will
enhance
our
ability
develop
effective
curative
interventions.
International Journal of Molecular Sciences,
Год журнала:
2021,
Номер
22(7), С. 3327 - 3327
Опубликована: Март 24, 2021
According
to
Darwin’s
theory,
endless
evolution
leads
a
revolution.
One
such
example
is
the
Clustered
Regularly
Interspaced
Palindromic
Repeats
(CRISPR)–Cas
system,
an
adaptive
immunity
system
in
most
archaea
and
many
bacteria.
Gene
editing
technology
possesses
crucial
potential
dramatically
impact
miscellaneous
areas
of
life,
CRISPR–Cas
represents
suitable
strategy.
The
has
ignited
revolution
field
genetic
engineering.
ease,
precision,
affordability
this
akin
Midas
touch
for
researchers
genomes.
Undoubtedly,
applications
are
endless.
extensively
employed
treatment
infectious
diseases,
metabolic
disorders,
curing
cancer,
developing
sustainable
methods
fuel
production
chemicals,
improving
quality
quantity
food
crops,
thus
catering
global
demands.
Future
will
provide
benefits
everyone
save
countless
lives.
evolving
rapidly;
therefore,
overview
continuous
improvement
important.
In
review,
we
aim
elucidate
current
state
tailor-made
format
from
its
discovery
exciting
breakthroughs
at
application
level
further
upcoming
trends
related
opportunities
challenges
including
ethical
concerns.
Bioscience Reports,
Год журнала:
2020,
Номер
40(4)
Опубликована: Март 24, 2020
Genome
editing
technologies,
particularly
those
based
on
zinc-finger
nucleases
(ZFNs),
transcription
activator-like
effector
(TALENs),
and
CRISPR
(clustered
regularly
interspaced
short
palindromic
repeat
DNA
sequences)/Cas9
are
rapidly
progressing
into
clinical
trials.
Most
use
of
to
date
has
focused
ex
vivo
gene
cells
followed
by
their
re-introduction
back
the
patient.
The
approach
is
highly
effective
for
many
disease
states,
including
cancers
sickle
cell
disease,
but
ideally
genome
would
also
be
applied
diseases
which
require
modification
in
vivo.
However,
technologies
can
confounded
problems
such
as
off-target
editing,
inefficient
or
delivery,
stimulation
counterproductive
immune
responses.
Current
research
addressing
these
issues
may
provide
new
opportunities
space.
In
this
review,
we
examine
current
status
scientific
basis
trials
featuring
ZFNs,
TALENs,
CRISPR-based
known
limitations
humans,
developing
engineering
space
that
should
lay
groundwork
further
translation
application.
Acta Pharmaceutica Sinica B,
Год журнала:
2021,
Номер
11(8), С. 2150 - 2171
Опубликована: Май 26, 2021
Within
less
than
a
decade
since
its
inception,
CRISPR-Cas9-based
genome
editing
has
been
rapidly
advanced
to
human
clinical
trials
in
multiple
disease
areas.
Although
it
is
highly
anticipated
that
this
revolutionary
technology
will
bring
novel
therapeutic
modalities
many
diseases
by
precisely
manipulating
cellular
DNA
sequences,
the
low
efficiency
of
vivo
delivery
must
be
enhanced
before
potential
can
fully
realized.
Here
we
discuss
most
recent
progress
CRISPR-Cas9
systems,
highlight
innovative
viral
and
non-viral
technologies,
emphasize
outstanding
challenges,
provide
updated
perspectives.
Frontiers in Immunology,
Год журнала:
2023,
Номер
14
Опубликована: Март 9, 2023
In
recent
years,
there
has
been
a
tremendous
development
of
biotechnological,
pharmacological,
and
medical
techniques
which
can
be
implemented
in
the
functional
modulation
immune
system
components.
Immunomodulation
attracted
much
attention
because
it
offers
direct
applications
both
basic
research
clinical
therapy.
Modulation
non-adequate,
amplified
response
enables
to
attenuate
course
disease
restore
homeostasis.
The
potential
targets
modulate
immunity
are
as
multiple
components
system,
thus
creating
various
possibilities
for
intervention.
However,
immunomodulation
faces
new
challenges
design
safer
more
efficacious
therapeutic
compounds.
This
review
cross-sectional
picture
currently
used
newest
pharmacological
interventions,
genomic
editing,
tools
regenerative
medicine
involving
immunomodulation.
We
reviewed
available
experimental
evidence
prove
efficiency,
safety,
feasibility
vitro
vivo.
also
advantages
limitations
described
techniques.
Despite
its
limitations,
is
considered
therapy
itself
or
an
adjunct
with
promising
results
developing
potential.
Proceedings of the National Academy of Sciences,
Год журнала:
2023,
Номер
120(19)
Опубликована: Май 1, 2023
Treatment
of
HIV-1
ADA
-infected
CD34+
NSG-humanized
mice
with
long-acting
ester
prodrugs
cabotegravir,
lamivudine,
and
abacavir
in
combination
native
rilpivirine
was
followed
by
dual
CRISPR-Cas9
C-C
chemokine
receptor
type
five
(CCR5)
proviral
DNA
gene
editing.
This
led
to
sequential
viral
suppression,
restoration
absolute
human
CD4
+
T
cell
numbers,
then
elimination
replication-competent
virus
58%
infected
mice.
Dual
CRISPR
therapies
enabled
the
excision
integrated
cells
contained
within
live
animals.
Highly
sensitive
nucleic
acid
nested
droplet
digital
PCR,
RNAscope,
outgrowth
assays
affirmed
elimination.
not
detected
blood,
spleen,
lung,
kidney,
liver,
gut,
bone
marrow,
brain
virus-free
Progeny
from
adoptively
transferred
CRISPR-treated
neither
nor
recovered.
Residual
fragments
were
easily
seen
untreated
viral-rebounded
No
evidence
off-target
toxicities
recorded
any
treated
Importantly,
therapy
demonstrated
statistically
significant
improvements
cure
percentages
compared
single
treatments.
Taken
together,
these
observations
underscore
a
pivotal
role
combinatorial
editing
achieving
infection.
PLoS Pathogens,
Год журнала:
2020,
Номер
16(6), С. e1008381 - e1008381
Опубликована: Июнь 11, 2020
HIV
invades
the
brain
during
acute
infection.
Yet,
it
is
unknown
whether
long-lived
infected
cells
release
productive
virus
that
can
egress
from
to
re-seed
peripheral
organs.
This
understanding
has
significant
implication
for
as
a
reservoir
and
most
importantly
interplay
between
Given
sheer
number
of
astrocytes
in
human
their
controversial
role
infection,
we
evaluated
infection
vivo
support
We
developed
two
novel
models
chimeric
astrocyte/human
blood
mononuclear
cells:
NOD/scid-IL-2Rgc
null
(NSG)
mice
(huAstro/HuPBMCs)
whereby
transplanted
(non-pseudotyped
or
VSVg-pseudotyped)
uninfected
primary
fetal
(NHAs)
an
astrocytoma
cell
line
(U138MG)
into
neonate
adult
NSG
reconstituted
animals
with
(PBMCs).
also
PBMCs
mimic
biological
course.
As
expected,
xenotransplanted
did
not
escape/migrate
out
barrier
(BBB)
was
intact
this
model.
demonstrate
organs,
at
least
part,
through
trafficking
CD4+
T
brain.
Astrocyte-derived
persists,
albeit
low
levels,
under
combination
antiretroviral
therapy
(cART).
Egressed
evolved
pattern
rate
typical
Lastly,
analysis
cortical
hippocampal
regions
donors
cART
revealed
harbor
0.4–5.2%
integrated
gag
DNA
2–7%
are
mRNA
positive.
These
studies
establish
paradigm
shift
dynamic
interaction
organs
which
inform
eradication
reservoirs.
