Trends in Molecular Medicine,
Journal Year:
2022,
Volume and Issue:
28(4), P. 319 - 330
Published: Feb. 14, 2022
The
impact
of
severe
acute
respiratory
syndrome
coronavirus
2
(SARS-CoV-2)
infection
during
pregnancy
on
the
developing
fetal
brain
is
poorly
understood.
Other
antenatal
infections
such
as
influenza
have
been
associated
with
adverse
neurodevelopmental
outcomes
in
offspring.
Although
vertical
transmission
has
rarely
observed
SARS-CoV-2
to
date,
given
potential
for
profound
maternal
immune
activation
(MIA),
likely.
Here
we
review
evidence
that
and
other
viral
can
result
maternal,
placental,
activation,
ultimately
offspring
morbidity.
Finally,
highlight
need
cellular
models
development
better
understand
short-
long-term
impacts
next
generation.
The Journal of Experimental Medicine,
Journal Year:
2021,
Volume and Issue:
218(3)
Published: Jan. 12, 2021
Although
COVID-19
is
considered
to
be
primarily
a
respiratory
disease,
SARS-CoV-2
affects
multiple
organ
systems
including
the
central
nervous
system
(CNS).
Yet,
there
no
consensus
on
consequences
of
CNS
infections.
Here,
we
used
three
independent
approaches
probe
capacity
infect
brain.
First,
using
human
brain
organoids,
observed
clear
evidence
infection
with
accompanying
metabolic
changes
in
infected
and
neighboring
neurons.
However,
for
type
I
interferon
responses
was
detected.
We
demonstrate
that
neuronal
can
prevented
by
blocking
ACE2
antibodies
or
administering
cerebrospinal
fluid
from
patient.
Second,
mice
overexpressing
ACE2,
neuroinvasion
vivo.
Finally,
autopsies
patients
who
died
COVID-19,
detect
cortical
neurons
note
pathological
features
associated
minimal
immune
cell
infiltrates.
These
results
provide
neuroinvasive
an
unexpected
consequence
direct
SARS-CoV-2.
Cell stem cell,
Journal Year:
2020,
Volume and Issue:
27(6), P. 951 - 961.e5
Published: Oct. 13, 2020
Coronavirus
disease
2019
(COVID-19),
caused
by
the
severe
acute
respiratory
syndrome
coronavirus
2
(SARS-CoV-2)
virus,
leads
to
symptoms
that
can
be
fatal.
However,
neurological
have
also
been
observed
in
some
patients.
The
cause
of
these
complications
is
currently
unknown.
Here,
we
use
human-pluripotent-stem-cell-derived
brain
organoids
examine
SARS-CoV-2
neurotropism.
We
find
expression
viral
receptor
ACE2
mature
choroid
plexus
cells
expressing
abundant
lipoproteins,
but
not
neurons
or
other
cell
types.
challenge
with
spike
pseudovirus
and
live
virus
demonstrate
tropism
for
epithelial
little
no
infection
glia.
infected
are
apolipoprotein-
ACE2-expressing
barrier.
Finally,
show
damages
epithelium,
leading
leakage
across
this
important
barrier
normally
prevents
entry
pathogens,
immune
cells,
cytokines
into
cerebrospinal
fluid
brain.
Frontiers in Neurology,
Journal Year:
2021,
Volume and Issue:
11
Published: Jan. 20, 2021
By
engaging
angiotensin-converting
enzyme
2
(ACE2
or
Ace2),
the
novel
pathogenic
severe
acute
respiratory
syndrome
coronavirus
(SARS-CoV-2)
invades
host
cells
and
affects
many
organs,
including
brain.
However,
distribution
of
ACE2
in
brain
is
still
obscure.
Here,
we
investigated
expression
by
analyzing
data
from
publicly
available
transcriptome
databases.
According
to
our
spatial
analysis,
was
relatively
highly
expressed
some
locations,
such
as
choroid
plexus
paraventricular
nuclei
thalamus.
cell-type
nuclear
found
neurons
(both
excitatory
inhibitory
neurons)
non-neuron
(mainly
astrocytes,
oligodendrocytes,
endothelial
cells)
human
middle
temporal
gyrus
posterior
cingulate
cortex.
A
few
ACE2-expressing
were
a
hippocampal
dataset,
none
detected
prefrontal
Except
for
additional
high
Ace2
olfactory
bulb
areas
well
pericytes
distribution,
mouse
similar
that
Thus,
results
reveal
an
outline
ACE2/Ace2
brains,
which
indicates
infection
SARS-CoV-2
may
be
capable
inducing
central
nervous
system
symptoms
disease
2019
(COVID-19)
patients.
Potential
species
differences
should
considered
when
using
models
study
neurological
effects
infection.
Proceedings of the National Academy of Sciences,
Journal Year:
2021,
Volume and Issue:
118(21)
Published: May 6, 2021
Prolonged
detection
of
severe
acute
respiratory
syndrome
coronavirus
2
(SARS-CoV-2)
RNA
and
recurrence
PCR-positive
tests
have
been
widely
reported
in
patients
after
recovery
from
COVID-19,
but
some
these
do
not
appear
to
shed
infectious
virus.
We
investigated
the
possibility
that
SARS-CoV-2
RNAs
can
be
reverse-transcribed
integrated
into
DNA
human
cells
culture
transcription
sequences
might
account
for
positive
PCR
seen
patients.
In
support
this
hypothesis,
we
found
copies
genome
infected
cells.
target
site
duplications
flanking
viral
consensus
LINE1
endonuclease
recognition
at
integration
sites,
consistent
with
a
retrotransposon-mediated,
target-primed
reverse
retroposition
mechanism.
also
found,
patient-derived
tissues,
evidence
suggesting
large
fraction
is
transcribed
sequences,
generating
viral-host
chimeric
transcripts.
The
may
thus
contribute
by
infection
clinical
recovery.
Because
detected
only
subgenomic
derived
mainly
3'
end
host
cell,
virus
cannot
produced
sequences.
Signal Transduction and Targeted Therapy,
Journal Year:
2021,
Volume and Issue:
6(1)
Published: Sept. 6, 2021
Abstract
SARS-CoV-2
has
been
reported
to
show
a
capacity
for
invading
the
brains
of
humans
and
model
animals.
However,
it
remains
unclear
whether
how
crosses
blood–brain
barrier
(BBB).
Herein,
RNA
was
occasionally
detected
in
vascular
wall
perivascular
space,
as
well
brain
microvascular
endothelial
cells
(BMECs)
infected
K18-hACE2
transgenic
mice.
Moreover,
permeability
vessel
increased.
Furthermore,
disintegrity
BBB
discovered
hamsters
by
administration
Evans
blue.
Interestingly,
expression
claudin5,
ZO-1,
occludin
ultrastructure
tight
junctions
(TJs)
showed
unchanged,
whereas,
basement
membrane
disrupted
Using
an
vitro
that
comprises
primary
BMECs
with
astrocytes,
found
infect
cross
through
BMECs.
Consistent
vivo
experiments,
MMP9
increased
collagen
IV
decreased
while
markers
TJs
were
not
altered
SARS-CoV-2-infected
Besides,
inflammatory
responses
including
vasculitis,
glial
activation,
upregulated
factors
occurred
after
infection.
Overall,
our
results
provide
evidence
supporting
can
transcellular
pathway
accompanied
without
obvious
alteration
TJs.
Cell stem cell,
Journal Year:
2020,
Volume and Issue:
27(6), P. 905 - 919.e10
Published: Oct. 21, 2020
Severe
acute
respiratory
syndrome
coronavirus
2
(SARS-CoV-2),
which
is
the
cause
of
a
present
pandemic,
infects
human
lung
alveolar
type
(hAT2)
cells.
Characterizing
pathogenesis
crucial
for
developing
vaccines
and
therapeutics.
However,
lack
models
mirroring
cellular
physiology
pathology
hAT2
cells
limits
study.
Here,
we
develop
feeder-free,
long-term,
three-dimensional
(3D)
culture
technique
derived
from
primary
tissue
investigate
infection
response
to
SARS-CoV-2.
By
imaging-based
analysis
single-cell
transcriptome
profiling,
reveal
rapid
viral
replication
increased
expression
interferon-associated
genes
proinflammatory
in
infected
cells,
indicating
robust
endogenous
innate
immune
response.
Further
tracing
mutations
acquired
during
transmission
identifies
full
individual
effectively
single
entry.
Our
study
provides
deep
insights
into
SARS-CoV-2
application
defined
3D
cultures
as
diseases.
Proceedings of the National Academy of Sciences,
Journal Year:
2022,
Volume and Issue:
119(35)
Published: Aug. 11, 2022
Although
increasing
evidence
confirms
neuropsychiatric
manifestations
associated
mainly
with
severe
COVID-19
infection,
long-term
dysfunction
(recently
characterized
as
part
of
"long
COVID-19"
syndrome)
has
been
frequently
observed
after
mild
infection.
We
show
the
spectrum
cerebral
impact
acute
respiratory
syndrome
coronavirus
2
(SARS-CoV-2)
ranging
from
alterations
in
mildly
infected
individuals
(orbitofrontal
cortical
atrophy,
neurocognitive
impairment,
excessive
fatigue
and
anxiety
symptoms)
to
damage
confirmed
brain
tissue
samples
extracted
orbitofrontal
region
(via
endonasal
transethmoidal
access)
who
died
COVID-19.
In
an
independent
cohort
26
COVID-19,
we
used
histopathological
signs
a
guide
for
possible
SARS-CoV-2
infection
found
that
among
5
exhibited
those
signs,
all
them
had
genetic
material
virus
brain.
Brain
these
five
patients
also
foci
replication,
particularly
astrocytes.
Supporting
hypothesis
astrocyte
neural
stem
cell-derived
human
astrocytes
vitro
are
susceptible
through
noncanonical
mechanism
involves
spike-NRP1
interaction.
SARS-CoV-2-infected
manifested
changes
energy
metabolism
key
proteins
metabolites
fuel
neurons,
well
biogenesis
neurotransmitters.
Moreover,
elicits
secretory
phenotype
reduces
neuronal
viability.
Our
data
support
model
which
reaches
brain,
infects
astrocytes,
consequently,
leads
death
or
dysfunction.
These
deregulated
processes
could
contribute
structural
functional
seen
brains
patients.
Cell stem cell,
Journal Year:
2021,
Volume and Issue:
29(2), P. 217 - 231.e8
Published: Dec. 25, 2021
Kidney
failure
is
frequently
observed
during
and
after
COVID-19,
but
it
remains
elusive
whether
this
a
direct
effect
of
the
virus.
Here,
we
report
that
SARS-CoV-2
directly
infects
kidney
cells
associated
with
increased
tubule-interstitial
fibrosis
in
patient
autopsy
samples.
To
study
effects
virus
on
independent
systemic
infected
human-induced
pluripotent
stem-cell-derived
organoids
SARS-CoV-2.
Single-cell
RNA
sequencing
indicated
injury
dedifferentiation
activation
profibrotic
signaling
pathways.
Importantly,
infection
also
led
to
collagen
1
protein
expression
organoids.
A
protease
inhibitor
was
able
ameliorate
by
Our
results
suggest
can
infect
induce
cell
subsequent
fibrosis.
These
data
could
explain
both
acute
COVID-19
patients
development
chronic
disease
long
COVID.
