A point-of-care biosensor for rapid detection and differentiation of COVID-19 virus (SARS-CoV-2) and influenza virus using subwavelength grating micro-ring resonator
Applied Physics Reviews,
Год журнала:
2023,
Номер
10(2)
Опубликована: Май 25, 2023
In
the
context
of
continued
spread
coronavirus
disease
2019
(COVID-19)
caused
by
SARS-CoV-2
and
emergence
new
variants,
demand
for
rapid,
accurate,
frequent
detection
is
increasing.
Moreover,
predominant
strain,
Omicron
variant,
manifests
more
similar
clinical
features
to
those
other
common
respiratory
infections.
The
concurrent
multiple
potential
pathogens
helps
distinguish
infection
from
diseases
with
overlapping
symptoms,
which
significant
providing
tailored
treatment
patients
containing
outbreak.
Here,
we
report
a
lab-on-a-chip
biosensing
platform
based
on
subwavelength
grating
micro-ring
resonator.
sensing
surface
functionalized
specific
antibody
against
spike
protein,
could
produce
redshifts
resonant
peaks
antigen–antibody
combination,
thus
achieving
quantitative
detection.
Additionally,
sensor
chip
integrated
microfluidic
featuring
an
anti-backflow
Y-shaped
structure
that
enables
two
analytes.
this
study,
realized
differentiation
COVID-19
influenza
A
H1N1.
Experimental
results
indicate
limit
our
device
reaches
100
fg/ml
(1.31
fM)
within
15
min
detecting
time,
cross-reactivity
tests
manifest
specificity
optical
diagnostic
assay.
Furthermore,
packaging
streamlined
workflow
facilitate
its
use
applications.
Thus,
presents
promising
approach
attaining
highly
sensitive,
selective,
multiplexed,
point-of-care
diagnosis
distinction
between
influenza.
Язык: Английский
Trivalent SARS-CoV-2 S1 Subunit Protein Vaccination Induces Broad Humoral Responses in BALB/c Mice
Vaccines,
Год журнала:
2023,
Номер
11(2), С. 314 - 314
Опубликована: Янв. 31, 2023
This
paper
presents
a
novel
approach
for
improving
the
efficacy
of
COVID-19
vaccines
against
emergent
SARS-CoV-2
variants.
We
have
evaluated
immunogenicity
unadjuvanted
wild-type
(WU
S1-RS09cg)
and
variant-specific
(Delta
S1-RS09cg
OM
S1
subunit
protein
delivered
either
as
monovalent
or
trivalent
antigen
in
BALB/c
mice.
Our
results
show
that
induced
broader
humoral
response
with
more
coverage
antigenically
distinct
variants,
especially
when
compared
to
Omicron-specific
S1.
was
also
found
increased
equivalent
ACE2
binding
inhibition,
IgG
endpoint
titer
at
early
timepoints,
spike
variants
Wuhan,
Delta,
Omicron
demonstrate
utility
provide
insights
into
impact
vaccine
approaches
on
immune
current
variant
landscape.
Particularly,
our
study
provides
insight
effects
further
increasing
valency
currently
approved
vaccines,
promising
protection
curtail
emerging
viral
Язык: Английский
The Long-Term Immunity of a Microneedle Array Patch of a SARS-CoV-2 S1 Protein Subunit Vaccine Irradiated by Gamma Rays in Mice
Vaccines,
Год журнала:
2025,
Номер
13(1), С. 86 - 86
Опубликована: Янв. 18, 2025
Background/Objectives:
COVID-19
vaccines
effectively
prevent
severe
disease,
but
unequal
distribution,
especially
in
low-
and
middle-income
countries,
has
led
to
vaccine-resistant
strains.
This
highlights
the
urgent
need
for
alternative
vaccine
platforms
that
are
safe,
thermostable,
easy
distribute.
study
evaluates
immunogenicity,
stability,
scalability
of
a
dissolved
microneedle
array
patch
(MAP)
delivering
rS1RS09
subunit
vaccine,
comprising
SARS-CoV-2
S1
monomer
RS09,
TLR-4
agonist
peptide.
Methods:
The
was
administered
via
MAP
or
intramuscular
injection
murine
models.
immune
responses
with
without
gamma
irradiation
as
terminal
sterilization
were
assessed
at
doses
5,
15,
45
µg,
alongside
neutralizing
antibody
Wuhan,
Delta,
Omicron
variants.
long-term
storage
stability
also
evaluated
through
protein
degradation
analyses
varying
temperatures.
Results:
elicited
stronger
ACE2-binding
inhibition
than
alone
trimer.
delivery
induced
sgnificantly
higher
longer-lasting
S1-specific
IgG
up
70
weeks
compared
injections.
Robust
Th2-prevalent
generated
all
groups
vaccinated
significant
antibodies
15
showing
dose-sparing
potential.
remained
stable
minimal
19
months
room
temperature
under
refrigeration,
regardless
gamma-irradiation.
After
an
additional
month
42
°C,
cit
showed
less
3%
degradation,
ompared
over
23%
liquid
Conclusions:
Gamma-irradiated
MAP-rS1RS09
is
promising
platform
stable,
scalable
production
eliminating
cold
chain
logistics.
These
findings
support
its
potential
mass
vaccination
efforts,
particularly
resource-limited
settings.
Язык: Английский
The recombinant spike S1 protein induces injury and inflammation in co-cultures of human alveolar epithelial cells and macrophages
PLoS ONE,
Год журнала:
2025,
Номер
20(2), С. e0318881 - e0318881
Опубликована: Фев. 10, 2025
The
current
lack
of
a
straightforward
and
convenient
modeling
approach
to
simulate
the
onset
acute
lung
injury
(ALI)
has
impeded
fundamental
research
hindered
screening
therapeutic
drugs
in
coronavirus
disease
2019
(COVID-19).
co-cultured
human
pulmonary
alveolar
epithelial
cells
(HPAEpics)
macrophages
(AMs)
were
exposed
complete
medium,
three
concentrations
recombinant
spike
S1
protein
(0.1,
1,
10
μg/mL),
or
lipopolysaccharide
(LPS)
(10
μg/mL).
harvested
at
2,
3
days
post-exposure.
Lactate
dehydrogenase
(LDH)
release,
IL-6,
TNF-ɑ,
malondialdehyde
(MDA)
production
quantified
compared.
Compared
those
co-cultures
HPAEpics
AMs
concentration
μg/mL
demonstrated
significantly
increased
levels
LDH
release
(22.9%
vs.
9.1%,
25.7%),
IL-6
(129
74,
110
pg/mg
protein),
TNF-ɑ
(75
51,
86
protein)
production,
similar
LPS.
However,
no
statistically
significant
differences
observed
MDA
production.
1
2
post-exposure,
post-exposure
exhibited
(23.4%
14.9%,
16.7%),
(127
81,
97
(5.6
3.2,
3.8
nmol/mg
but
lower
(58
79
than
After
exposure,
showed
(25.3%
18.4%),
(5.5
4.3
compared
monocultures,
13.8%),
(139
98
4.7
decreased
(59
95
monocultures.
Conclusions:
exposure
induced
inflammation
This
methodology
for
establishing
COVID-19-associated
ALI
model
may
have
promising
potential
applications
value.
Язык: Английский
Fourth dose of microneedle array patch of SARS-CoV-2 S1 protein subunit vaccine elicits robust long-lasting humoral responses in mice
International Immunopharmacology,
Год журнала:
2024,
Номер
129, С. 111569 - 111569
Опубликована: Фев. 9, 2024
Язык: Английский
Tetravalent SARS-CoV-2 S1 subunit protein vaccination elicits robust humoral and cellular immune responses in SIV-infected rhesus macaque controllers
mBio,
Год журнала:
2023,
Номер
14(5)
Опубликована: Окт. 13, 2023
ABSTRACT
The
coronavirus
disease
2019
(COVID-19)
pandemic
has
highlighted
the
need
for
safe
and
effective
vaccines
to
be
rapidly
developed
distributed
worldwide,
especially
considering
emergence
of
new
severe
acute
respiratory
syndrome
2
(SARS-CoV-2)
variants.
Protein
subunit
have
emerged
as
a
promising
approach
due
their
proven
safety
record
ability
elicit
robust
immune
responses.
In
this
study,
we
evaluated
immunogenicity
efficacy
an
adjuvanted
tetravalent
S1
protein
COVID-19
vaccine
candidate
composed
Wuhan,
B.1.1.7
variant,
B.1.351
P.1
variant
spike
proteins
in
nonhuman
primate
model
with
controlled
SIVsab
infection.
induced
both
humoral
cellular
responses,
T
B
cell
responses
mainly
peaking
post
boost
immunization.
also
elicited
neutralizing
cross-reactive
antibodies,
angiotensin-converting
enzyme
(ACE2)-blocking
including
spike-specific
CD4
+
cells.
Importantly,
was
able
generate
Omicron
spike-binding
ACE2-blocking
antibodies
without
specifically
vaccinating
Omicron,
suggesting
potential
broad
protection
against
emerging
composition
significant
implications
development
implementation,
providing
antibody
numerous
SARS-CoV-2
IMPORTANCE
study
provides
important
insights
into
(SARS-CoV-2).
primates
SIVagm
infection
variant-specific
Omicron.
These
findings
suggest
that
could
provide
multiple
variants
while
minimizing
risk
escape
Additionally,
use
rhesus
macaques
may
better
represent
humans
chronic
viral
diseases,
highlighting
importance
preclinical
animal
models
development.
Overall,
valuable
information
implementation
vaccines,
particularly
achieving
global
equity
addressing
Язык: Английский
Second Boost of Omicron SARS-CoV-2 S1 Subunit Vaccine Induced Broad Humoral Immune Responses in Elderly Mice
bioRxiv (Cold Spring Harbor Laboratory),
Год журнала:
2024,
Номер
unknown
Опубликована: Фев. 6, 2024
Currently
approved
COVID-19
vaccines
prevent
symptomatic
infection,
hospitalization,
and
death
from
the
disease.
However,
repeated
homologous
boosters,
while
considered
a
solution
for
severe
forms
of
disease
caused
by
new
SARS-CoV-2
variants
in
elderly
individuals
immunocompromised
patients,
cannot
provide
complete
protection
against
breakthrough
infections.
This
highlights
need
alternative
platforms
booster
vaccines.
In
our
previous
study,
we
assessed
boost
effect
Beta
S1
recombinant
protein
subunit
vaccine
(rS1Beta)
aged
mice
primed
with
an
adenovirus-based
expressing
SARS-CoV-2-S1
(Ad5.S1)
via
subcutaneous
injection
or
intranasal
delivery,
which
induced
robust
humoral
immune
responses
(1).
this
follow-up
demonstrated
that
second
dose
non-adjuvanted
Omicron
(BA.1)
Toll-like
receptor
4
(TLR4)
agonist
RS09
(rS1RS09OM)
was
effective
stimulating
strong
S1-specific
inducing
significantly
high
neutralizing
antibodies
Wuhan,
Delta,
100-week-old
mice.
Importantly,
elicits
cross-reactive
antibody
responses,
resulting
ACE2
binding
inhibition
spike
variants,
including
its
subvariants.
Interestingly,
levels
IgG
correlated
level
serum
samples,
although
showed
weaker
correlation
compared
to
Wuhan
level.
Furthermore,
immunogenic
properties
rS1
young,
middle-aged,
mice,
reduced
immunogenicity
age,
especially
impaired
Th1-biased
response
Our
findings
demonstrate
variant
concern
(VOC)
as
has
potential
offer
cross-neutralization
broad
range
improve
effectiveness
newly
emerging
who
were
previously
authorized
Язык: Английский
Long-term Immunity of a Microneedle Array Patch of SARS-CoV-2 S1 Protein Subunit Vaccine Irradiated by Gamma Rays in Mice
bioRxiv (Cold Spring Harbor Laboratory),
Год журнала:
2024,
Номер
unknown
Опубликована: Окт. 25, 2024
Abstract
COVID-19
vaccines
effectively
prevent
symptomatic
infection
and
severe
disease,
including
hospitalization
death.
However,
unequal
vaccine
distribution
during
the
pandemic,
especially
in
low-
middle-income
countries,
has
led
to
emergence
of
vaccine-resistant
strains.
This
underscores
need
for
alternative,
safe,
thermostable
platforms,
such
as
dissolved
microneedle
array
patches
(MAP)
delivering
a
subunit
vaccine,
which
eliminate
cold
chain
trained
healthcare
personnel.
study
demonstrates
that
SARS-CoV-2
S1
monomer
with
RS09,
TLR-4
agonist
peptide,
serves
an
optimal
protein
immunogen.
combination
stimulates
stronger
S1-specific
immune
response,
resulting
binding
membrane-bound
spike
on
cell
surface
ACE2-binding
inhibition,
compared
alone
or
trimer
S1,
regardless
RS09.
MAP
delivery
rS1RS09
elicited
higher
longer-lasting
immunity
conventional
intramuscular
injection.
IgG
levels
remained
significantly
elevated
up
70
weeks
post-administration.
Additionally,
different
doses
5,
15,
45
μ
g
induced
robust
sustained
Th2-prevalent
responses,
suggesting
dose-sparing
effect
inducing
high
neutralizing
antibodies
against
Wuhan,
Delta,
Omicron
variants
at
15
dose.
Moreover,
gamma
irradiation
terminal
sterilization
method
did
not
affect
immunogenicity,
irradiated
maintaining
comparable
efficacy
non-irradiated
ones.
The
stability
was
evaluated
after
long-term
storage
room
temperature
refrigeration
19
months,
showing
minimal
degradation.
Further,
additional
one-month
(42°C),
both
degraded
less
than
3%,
while
liquid
over
23%.
Overall,
these
results
indicate
sterilized
MAP-rS1RS09
maintain
extended
without
refrigeration,
supporting
their
potential
mass
production
widespread
use
global
vaccination
efforts.
Язык: Английский
Tetravalent SARS-CoV-2 S1 Subunit Protein Vaccination Elicits Robust Humoral and Cellular Immune Responses in SIV-Infected Rhesus Macaque Controllers
bioRxiv (Cold Spring Harbor Laboratory),
Год журнала:
2023,
Номер
unknown
Опубликована: Март 16, 2023
The
COVID-19
pandemic
has
highlighted
the
need
for
safe
and
effective
vaccines
to
be
rapidly
developed
distributed
worldwide,
especially
considering
emergence
of
new
SARS-CoV-2
variants.
Protein
subunit
have
emerged
as
a
promising
approach
due
their
proven
safety
record
ability
elicit
robust
immune
responses.
In
this
study,
we
evaluated
immunogenicity
efficacy
an
adjuvanted
tetravalent
S1
protein
vaccine
candidate
composed
Wuhan,
B.1.1.7
variant,
B.1.351
P.1
variant
spike
proteins
in
nonhuman
primate
model
with
controlled
SIVsab
infection.
induced
both
humoral
cellular
responses,
T-
B
cell
responses
mainly
peaking
post-boost
immunization.
also
elicited
neutralizing
cross-reactive
antibodies,
ACE2
blocking
T-cell
including
specific
CD4+
T
cells.
Importantly,
was
able
generate
Omicron
binding
antibodies
without
specifically
vaccinating
Omicron,
suggesting
potential
broad
protection
against
emerging
composition
significant
implications
development
implementation,
providing
antibody
numerous
Язык: Английский
Fourth dose of Microneedle Array Patch of SARS-CoV-2 S1 Protein Subunit Vaccine Elicits Robust Long-lasting Humoral Responses in mice
bioRxiv (Cold Spring Harbor Laboratory),
Год журнала:
2023,
Номер
unknown
Опубликована: Окт. 5, 2023
Abstract
The
COVID-19
pandemic
has
underscored
the
pressing
need
for
safe
and
effective
booster
vaccines,
particularly
in
considering
emergence
of
new
SARS-CoV-2
variants
addressing
vaccine
distribution
inequalities.
Dissolving
microneedle
array
patches
(MAP)
offer
a
promising
delivery
method,
enhancing
immunogenicity
improving
accessibility
through
skin’s
immune
potential.
In
this
study,
we
evaluated
patch-based
S1
subunit
protein
candidate,
which
comprised
bivalent
formulation
targeting
Wuhan
Beta
variant
alongside
monovalent
Delta
spike
proteins
murine
model.
Notably,
second
boost
homologous
MAP-S1(WU+Beta)
induced
15.7-fold
increase
IgG
endpoint
titer,
while
third
heterologous
MAP-S1RS09Delta
yielded
more
modest
1.6-fold
increase.
Importantly,
study
demonstrated
that
administration
four
doses
MAP
robust
long-lasting
responses,
persisting
at
least
80
weeks.
These
responses
encompassed
various
isotypes
remained
statistically
significant
one
year.
Furthermore,
neutralizing
antibodies
against
multiple
were
generated,
with
comparable
observed
Omicron
variant.
Overall,
these
findings
emphasize
potential
MAP-based
vaccines
as
strategy
to
combat
evolving
landscape
deliver
worldwide.
Язык: Английский