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Title: AlooDenish

1

SARS-CoV-2 and COVID-19
A presentation by
Aloo Denish
(Biochemist Microbiologist)
Chuka University CSI International Ltd
E-mail aloo.denish3_at_gmail.com
... if you know your enemies and know yourself,
you will not be imperiled in a hundred battles.
Sun Tzu, The Art of War

Note Before proceeding with reading this
resourceful document, kindly listen to the
message in the following 3 links
Link 1 https//youtu.be/Y-NEq6TjsL0
Link 2 https//www.facebook.com/100006451518515/v
ideos/826467281352378/
Link 3 https//www.linkedin.com/posts/aloodenis
h_covid-19-genomic-organization-life-cycle-activit
y-6848906155129892864-8KnN

3
1.0 History - Did you Know?

In the past, the world has faced respiratory
disease pandemics
The 1918 H1N1 (Spanish flu) -50 million deaths
worldwide
The 1957 H2N2 (Asian flu) -14 million deaths
worldwide
The 1968 H3N2 (Hong Kong flu) -14 million deaths
worldwide
The 2005 H5N1 (Bird flu)
The 2009 H1N1 (Swine flu)- 151,700575,400 deaths
worldwide
2001 to 2003 severe acute respiratory syndrome
(SARS)
2012 to 2015 Middle East respiratory syndrome
(MERS)
December 2019 Novel coronavirus 2019
(SARS-CoV-2) that causes Covid-19 discovered in
Wuhan city, Hubei Province, China

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2.0 Definition

Coronaviruses (CoVs) are enveloped,
positive-sense, single-stranded RNA viruses that
belong to the subfamily Coronavirinae, family
Coronavirdiae, order Nidovirales.
There are four genera of CoVs, namely,
Alphacoronavirus (aCoV), Betacoronavirus (ßCoV),
Deltacoronavirus (dCoV), and Gammacoronavirus
(?CoV)
Severe acute respiratory syndrome coronavirus 2
(SARS-CoV-2) is the virus that causes COVID-19
(coronavirus disease 2019), the respiratory
illness responsible for the COVID-19
Coronavirus disease (COVID-19) is an infectious
disease caused by the SARS-CoV-2 virus.

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3.0 Taxonomy of SARS-CoV-2

(unranked) Virus
Realm Riboviria
Kingdom Orthornavirae
Phylum Pisuviricota
Class Pisoniviricetes
Order Nidovirales
Family Coronaviridae
Genus Betacoronavirus
Subgenus Sarbecovirus
Species Severe acute respiratory
syndromerelated coronavirus
Virus Severe acute respiratory syndrome
coronavirus 2

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3.1 Variants of SARS-CoV-2

There are many thousands of variants of
SARS-CoV-2, which can be grouped into the much
larger clades.
The World Health Organization has currently
(2021) declared four variants of concern, with
evidence of increased transmissibility and
virulence, alongside changes to antigenicity,
which are as follows
Alpha Lineage B.1.1.7 emerged in the United
Kingdom in September 2020. Notable mutations
include N501Y and P681H. An E484K mutation in
some lineage B.1.1.7 virions has been noted
Beta Lineage B.1.351 emerged in South Africa in
May 2020. Notable mutations include K417N, E484K
and N501Y.
Gamma Lineage P.1 emerged in Brazil in November
2020. Notable mutations also include K417N, E484K
and N501Y.
Delta Lineage B.1.617.2 emerged in India in
October 2020.
Other variants include Lambda (lineage C.37), Mu
(lineage B.1.621), Epsilon (lineages B.1.429,
B.1.427, CAL.20C), Zeta (lineage P.2), Theta
(lineage P.3), Eta (lineage B.1.525), Iota
(lineage B.1.526), Kappa (lineage B.1.617.1),
e.t.c.

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4.0 Structure of SARS-CoV-2

Spherical, enveloped, around 80120 nm in
diameter, with multiple outwardly projected
club-like homotrimeric, glycosylated S proteins
imparting them incredible appearance of a solar
corona, prompting their popular name, CoVs.
Enclosed within the lipid bilayer envelope of the
virion is helically symmetrical nucleocapsids
comprising complex of ssRNA and capsid proteins.
There are four important structural
proteinsspike (S), membrane (M), envelope (E),
and nucleocapsid (N) proteinsthat are encoded by
structural genes located within the region
preceeding 30 end of genome.
There are several non-structural and accessory
proteins, which together are responsible for the
structural and functional aspects of virus

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5.0 Genome Organization

SARS-CoV-2 is a positive-sense single-stranded
RNA (ssRNA) virus, with a single linear RNA
segment.
Genome size ranges from 26 to 32 kb and comprise
611 open reading frames (ORFs) encoding 9680
amino acid polyproteins (Guo et al. 2020).
Genome has highest composition of U (32.2),
followed by A (29.9), and a similar composition
of G (19.6) and C (18.3). The nucleotide bias
arises from the mutation of guanines and
cytosines to adenosines and uracils,
respectively.
The first ORF (ORF1a and ORF1b) comprises
approximately 67 of the genome that encodes 16
non-structural proteins (nsps), whereas the
remaining ORFs encode for accessory proteins and
structural proteins.
Accessory genes are interspersed between the
structural genes and contain at least nine ORFs
for accessory proteins.
Its genome lacks the hemagglutinin-esterase gene.
However, it comprises two flanking untranslated
regions (UTRs) at 5' end of 265 and 3' end of 358
nucleotides.

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6.0 Description of Structural Organization

Non-structural proteins
Structural Proteins
Accessory proteins

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6.1 Non-structural proteins

The initial two-thirds of the RNA sequence encode
the two main transcriptional units, ORF1a and
ORF1ab these units encode two polyproteins (PP1a
and PP1ab, respectively).
The pp1a non-structural protein corresponds to
NSP1 to NSP11 and pp1ab non-structural protein
comprises of NSP12 to NSP16
The larger unit, PP1ab, contains ORFs for at
least 16 non-structural proteins (Nsp1-16)
The non-structural proteins have various
functions in biological phenomena that are
important for the virus such as replication,
correction of replication errors
(proofreading), translation, suppression of
host proteins, immune response blockage, and RNA
stabilization.

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S.No Name Protein (Full Name) and function
1 nsp1 N-terminal product of the viral replicase -gt acts as host translation inhibitor and also degrade host mRNAs
2 nsp2 N-terminal product -gtBinds to prohibitin 1 and prohibitin 2 (PHB1 and PHB2)
3 nsp3 Papain-like proteinase -gt Responsible for release of NSP1, NSP2, and NSP3 from the N-terminal region of pp1a and 1ab
4 nsp4 Membrane-spanning protein containing Transmembrane domain 2 -gtInvolves in double-membrane vesicle formation
5 nsp5 Proteinase and main proteinase -gtInhibits IFNsignaling
6 nsp6 Putative transmembrane domain -gtInduces formation of ER-derived autophagosomes
7 nsp7 RNA-dependent RNA polymerase - Acts as a cofactor with nsp8 and nsp12
8 nsp8 Multimeric RNA polymerase replicase single-stranded -gtMakes heterodimer with NSP8 and 12
9 nsp9 RNA-binding viral protein -gtInvolves in dimerization and RNA binding
10 nsp10 Growth-factor-like protein possessing two zinc binding motifs -gtacts as a scaffold protein for nsp14 and nsp16
11 nsp11 short peptide at the end of orf1a -gt Unclear function
12 nsp12 RNA-dependent RNA polymerase gtfor replication and methylation
13 nsp13 Helicase -gt Helicase core domain binds ATP. Zinc-binding domain is involved in replication and transcription
14 nsp14 Exoribonuclease domain (ExoN/nsp14) -gtExoribonuclease activity and N7-guanine methyltransferase activity
15 nsp15 EndoRNAse nsp15-A1 and nsp15B-NendoU -gt Mn(2 )-dependent endoribonuclease activity
16 nsp16 2-O-MT 2-O-ribose methyltransferase -gtmediates mRNA cap 20-O-ribose methylation
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6.2 Structural Proteins

The structural genes encode the structural
proteins, spike (S), envelope (E), membrane (M),
and nucleocapsid (N).
6.2.1 The S protein
The total length of SARS-CoV-2 S is 1273 aa and
consists of a signal peptide (amino acids 113)
located at the N-terminus, the S1 subunit (14685
residues), and the S2 subunit (6861273 residues)
The S1 subunit and S2 subunit are responsible for
receptor binding and membrane fusion,
respectively.
The S1 subunit comprises an N-terminal domain
(14305 residues) and a receptor-binding domain
(RBD, 319541 residues).
The S2 subunit comprises the fusion peptide (FP)
(788806 residues), heptapeptide repeat sequence
1 (HR1) (912984 residues), HR2 (11631213
residues), TM domain (12131237 residues), and
cytoplasm domain (12371273 residues).
SARS-CoV-2 S harbors a furin cleavage site
(682685 residues) at the S1/S2 boundary, which
may increase the efficiency of SARS-CoV-2
transmission

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6.2.2 Envelope (E) protein
The smallest amongst all the structural proteins,
around 812 kDa.
Function plays major role in pathogenesis,
virus assembly, and release .
6.2.3 Membrane (M) protein
n is O-linked glycoprotein of around 2530 kDa,
and is most abundant amongst various structural
proteins, and possesses three distinct
transmembrane domains .
The homodimeric M protein associates with other
viral structural proteins, including
nucleocapsid, facilitating the molecular assembly
of virus particles as well as may be involved
during pathogenesis.
6.2.4 Nucleocapsid (N) protein
It distinctly possesses three highly conserved
domains an N-terminal domain, an RNA-binding
domain or a linker region, and a C-terminal
domain.
It has been observed that these three domains
may together orchestrate RNA binding and its
phosphorylated status is prerequisite for
triggering a structural dynamism facilitating the
affinity for viral versus non-viral RNA .
Participates in RNA packaging in a
beads-on-a-string type conformation. In addition
to be involved in organization of viral genome, N
protein also facilitates virion assembly and
enhances virus transcription efficiency amongst
others

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6.3 Accessory Factors

There are nine accessory proteinsORF3a, 3d, 6,
7a, 7b, 8, 9b, 14, and 10produced from at least
five ORFs encoding accessory genes (ORF3a, ORF6,
ORF7a, ORF7b, and ORF8), novel overlapping ORF3d
(earlier known as 3b), leaky scanning of sgRNA of
N gene (ORF9b and 14), and ORF10 from downstream
of N gene.
Accessory proteins play a crucial role in virus
replication
They may also be involved in host immune escape.
these proteins play an important role in
interactions between the virus and host,
including modulating and blocking the production
of pro-inflammatory cytokines

6.3.1 ORF3a and ORF3d Proteins
Accessory factor 3a is encoded by ORF3a located
in between the S and E genes, and is the largest
accessory proteins of SARS-CoV-2, consisting of
274 amino acid residues.
ORF3a forms dimer and its six transmembrane
helices together create ion channelin the host
cell membrane, which is highly conducive for
Ca2/K cations compared to Na ion. It is also
involved in virus release, apoptosis and
pathogenesis.
ORF3d encodes 3d protein which consists of
154-aa long polypeptide chain, and is found to be
located in the nucleolus and mitochondria.
6.3.2 ORF6 Protein
A 61-amino acid long membrane-associated protein.

6.3.3 ORF7a and ORF7b Proteins
Synthesized from the bicistronic subgenomic RNA 7
of SARS-CoV-2.
The 122-aa ORF7a protein is a type-I
transmembrane protein containing a 15 aa signal
peptide sequence, an 81aa luminal domain, 21aa
transmembrane domain and a short C-terminal tail.
The ORF7b protein consists of 44-amino acids, and
is an integral membrane protein, expressed in
SARS-CoV-infected cells wherein it remains
localized in the Golgi compartment
6.3.4 ORF8 Protein
Consists of 121 amino acid residues.
Has been found to interact with major
histocompatibility complex-I (MHC-I), thereby
mediating their degradation in cell culture, and
therefore may help in immune evasion

6.3.5 ORF9b Protein
Consists of 97 amino acid residues, and is
probably expressed by leaky scanning of sgRNA of
N gene.
Tends to associate with adaptor protein, TOM70,
and therby suppress IFN-I mediated antiviral
response
6.3.6 ORF10 Protein
Encoding by gene predicted to be located
downstream of the N gene
6.3.7 ORF14 Protein
Made up of 73 amino acid residues, and is also
likely to be synthesized by leaky scanning of
sgRNA of N gene. However, its function is not
clearly understood.

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7.0 Mutations

Mutation on the spike protein -Mutation
23403AgtG-(D614G)
Mutation on the NSP12 protein -Mutation
14408CgtT-(P323L)
Mutation on the ORF3a protein -Mutation
25563GgtT-(Q57H)
Mutation on the NSP2 protein -mutation
1059CgtT-(T85I)
Mutations on the NSP13 protein
Mutations on the ORF8 protein -two high-frequency
mutations, 28144TgtC-(L84S) and 27964CgtT-(S24L)
Mutations on the nucleocapsid protein -high
frequency mutations, 28881GgtA, 28881GgtA, and
28883GgtC.

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8.0 Life Cycle of SARS-CoV-2

Involves cellular invasion of virus, expression
of viral genes, and formation of progeny and
eventual exit.
Involves
Attachment to Host Cell Surface, Penetration and
Uncoating
Replication-Transcription Complex (RTC)
Formation
Synthesis of Viral RNA
Molecular Assembly and Release of SARS-CoV-2

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8.1 Attachment to Host Cell Surface,
Penetration and Uncoating.

The spike (S) protein, via its receptor binding
domain (RBD), attaches to angiotensin converting
enzyme 2 (ACE2) receptors that is found on the
surface of many human cells, including those in
the lungs allowing virus entry.
The S protein is subjected to proteolytic
cleavages by host proteases (i.e. trypsin and
furin), in two sites located at the boundary
between the S1 and S2 subunits (S1/S2 site).
In a later stage happens the cleavage of the S2
domain (S2'site) in order to release the fusion
peptide. This event will trigger the activation
of the membrane fusion mechanism. Typically,
human cell ingests the virus in a process called
endocytosis

Once entered the cytoplasm, it has been suggested
most likely that COVID-19 employs a unique
three-step method for membrane fusion, involving
receptor-binding and induced conformational
changes in Spike (S) glycoprotein followed by
cathepsin L proteolysis through intracellular
proteases and further activation of membrane
fusion mechanism within endosomes (Simmons et
al., 2005).
Then, the endosome opens to release virus to the
cytoplasm, and uncoating of viral nucleocapsid
(N) is started via proteasomes which typically
can hydrolyse endogenous proteins, but they are
also capable of degrading exogenous proteins such
as the SARS nucleocapsid protein (Q. Wang et al.,
2010).
A different two-step mechanism has been suggested
(Li, 2016) and in this case the virion binds to a
receptor on the target host cell surface through
its S1 subunit and the Spike is cleaved by host
proteases (Hasan et al., 2020) and then it is
expected the fusion at low pH between viral and
host target membranes via S2 subunit.
Finally, the viral genetic material a single
stranded RNA is fully released into the
cytoplasm.

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8.2 Replication-Transcription Complex (RTC)
Formation

Immediately after release of viral nucleocapsid,
ssRNA serves as functional mRNA with respect to
ORF1a and ORF1b encoding polyprotein pp1a
(440500 kDa) and pp1ab (740810 kDa),
respectively.
pp1a is 1.22.2 folds more expressed compared to
pp1ab dueto differential efficiency of frameshift
between ORF1a and ORF1b genes.
These two polyproteins undergo autoproteolytic
processing yielding 16 nsps, which together form
the RTC for viral RNA synthesis.
This functional RTC results into formation of a
nested set of sgRNAs via discontinuous
transcription.

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8.3 Synthesis of Viral RNA

The formation of RTC sets molecular process in
motion leading to synthesis of multiple copies
of viral RNA.
These -ssRNA (negative ssRNA) serves as
intermediate template.
Meanwhile, polymerase switches template at short
motifs, transcription regulated sequences (TRS)
during -ssRNA synthesis, thereby producing a
multiple 50-nested set of negative sense sgRNAs
which, in turn, used as templates to form a
30-nested set of positive sense sgRNAs.
Thereafter, they associate with host ribosome,
synthesizing various structural and accessory
proteins building multiple virus structure .

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8.4 Molecular Assembly and Release of
SARS-CoV-2

Most of the structural and accessory proteins
associated with membrane such as S, M, and E are
synthesized by endoplasmic reticulum-bound
ribosomes, whereas other viral proteins,
including N protein, are translated by free
cytosolic ribosomes of host cells.
In addition, these structural proteins also
undergo posttranslational modification that
modulate their functions.
The assembly of virion converges at site of
endoplasmic reticulumGolgi intermediate
compartment (ERGIC), wherein M protein provides
scaffold and orchestrate virion morphogenesis by
heterotypic interaction with other structural
proteins, such as M-S and M-E, thereby
facilitating molecular incorporation.
Furthermore, M-N interactions mediates
condensation of the nucleocapsid with the
envelope along with E protein.
Post molecular assembly, progeny virions are
transported in smoothwall vesicle and using
secretory pathway they are trafficked to plasma
membrane and eventually exit though exocytosis
and spread to other parts of body

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9.0 Transmission

Covid-19 is a contagious viral infection that can
be spread through inhalation or ingestion of
viral respiratory droplets as a result of
? Coughing ?Sneezing
?Talking/singing ?Sharing airspace 30
minutes infects
? Touching infected surfaces are primary sources
of infection.
Silent spreaders of Covid-19
Asymptomatic patients carry active virus in
their body but never develop any symptoms.
Pauci-symptomatic (Mild) patients Feel a little
unwell from covid-19 infection but continue to
come into close contact with others.
Pre-symptomatic patients Infected and are
incubating the virus but no symptoms.
Children are not immune from this infection and
their symptoms dont correlate with exposure and
infection.

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10.0 PATHOPHYSIOLOGY

10.1 Asymptomatic Phase
The inhaled virus SARS-CoV-2 binds to epithelial
cells in the nasal cavity via angiotensin
converting enzyme 2 (ACE2).
In vitro data with SARS-CoV indicate that the
ciliated cells are primary cells infected in the
conducting airways.
The virus undergoes local replication and
propagation, along with the infection of ciliated
cells in the conducting airways.
This stage lasts a couple of days and the innate
immune response generated during this phase is a
limited one.
In spite of having a low viral load at this
time, the individuals are highly infectious and
the virus can be detected via nasal swab testing.

10.2 Invasion and Infection of the Upper
Respiratory Tract
The virus propagates and migrates from the nasal
epithelium to the upper respiratory tract via the
conducting airways and a more robust innate
immune response is triggered.
Nasal swabs or sputum should yield the virus
(SARS-CoV-2) as well as early markers of the
innate immune response.
Due to the involvement of the upper airways, the
disease manifests with symptoms of fever, malaise
and dry cough.
There is a greater immune response during this
phase involving the release of C-X-C motif
chemokine ligand 10 (CXCL-10) and interferons
(IFN-ß and IFN-?) from the virus-infected cells.
The majority of patients do not progress beyond
this phase as the mounted immune response is
sufficient to contain the spread of infection.
For about 80 of the infected patients, the
disease will be mild and mostly restricted to the
upper and conducting airways. These individuals
may be monitored at home with conservative
symptomatic therapy.

10.3 Involvement Of The Lower Respiratory Tract
And Progression To Acute Respiratory Distress
Syndrome (ARDS)
- Hypoxia, ground glass infiltrates/opacity and
progression to ARDS
About 20 of all infected patients progress to
this stage of disease and develop severe
symptoms.
The virus invades and enters the type 2 alveolar
epithelial cells via the host receptor ACE-2 and
starts to undergo replication to produce more
viral Nucleocapsids.
The virus-laden pneumocytes now release many
different cytokines and inflammatory markers such
as interleukins (IL-1, IL-6, IL-8, IL-120 and
IL-12), tumour necrosis factor-a(TNF-a), IFN-?
and IFN-ß, CXCL-10, monocyte chemoattractant
protein-1 (MCP-1) and macrophage inflammatory
protein-1a (MIP-1a).
This cytokine storm acts as a chemoattractant
for neutrophils, CD4 helper T cells and CD8
cytotoxic T cells, which then begin to get
sequestered in the lung tissue. These cells are
responsible for fighting off the virus, but in
doing so are responsible for the subsequent
inflammation and lung injury.
The host cell undergoes apoptosis with the
release of new viral particles, which then infect
the adjacent type 2 alveolar epithelial cells in
the same manner.
Due to the persistent injury caused by the
sequestered inflammatory cells and viral
replication leading to loss of both type 1 and
type 2 pneumocytes, there is diffuse alveolar
damage eventually culminating in an acute
respiratory distress syndrome

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11.0 Symptoms of COVID-19

COVID-19 affects different people in different
ways. Most infected people will develop mild to
moderate illness and recover without
hospitalization.
Most common symptoms
?Fever ?cough
?Tiredness ?loss of taste or smell.
Less common symptoms
?sore throat ?headache ?aches
and pains ?diarrhoea
?a rash on skin, or discolouration of fingers or
toes ? red or irritated eyes.
Serious symptoms
?difficulty breathing or shortness of breath
?loss of speech or mobility, or confusion
? chest pain.
On average it takes 56 days from when someone is
infected with the virus for symptoms to show,
however it can take up to 14 days.

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11.1 Covid-19 complications

?Acute respiratory failure (ARF) ?Acute
respiratory distress syndrome (ARDS)
?Acute liver injury
?Septic shock
?Acute kidney injury
? Rhabdomyolysis
?Acute cardiac injury
? Acute brain injury
?Pneumonia pulmonary embolism followed by
extra-pulmonary systemic hyperinflammation
syndrome.
?Adipose tissue increased fat composition
sustained fat loss in recovered patients,
elevated plasma F.As and TAGs (hyperlipidemia).
A?cute Pancreas injury contribute to
long-lasting diabetes. Insulin resistance,
hyperglycemia, altered glucose metabolism
development of T2D.
?Disseminated intravascular coagulation/blood
clots hypertension.
?Secondary infections Strep and Staph that
raises the risk of death.
?Multisystem inflammatory syndrome in children
(MIS-C)

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12.0 COVID-19 Diagnosis

Clinical features e.g fever, fatigue, Dry cough,
breathlessness etc
Screening Laboratory Tests hematologic,
biochemical inflammatory biomarkers etc.
Imaging chest x-ray, CT scan
Molecular Examination RT-PCR, Quantitative
RT-PCR etc.
Immunological Assays ELISA, CLIA, IFA etc.
Novel Techniques- Next generation sequencing,
CRISPR, LAMP etc.

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13.0 Treatment

To date, no single medication has been reported
or proposed to combat the infective viral load of
SARS-CoV-2.
However, previous strategies for developing
proper medications to pulverize SARS-CoV can be
extrapolated to COVID-19 infection effectively.
Scientists, several research groups, and
clinicians across the globe are working towards
finding effective medications that can curtail or
eliminate the viral load of SARS-CoV-2.
Below is a list of natural products/isolated
compounds or their derivatives and drugs that
inhibit the coronavirus family

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Categories Compound Name Proposed Mode of Actions Involved Viruses
Antiviral drugs Remdesivir ( GS-5734, Nucleoside analogue of Remdesivir triphosphate) ( RDV-TP ) Inhibitor of RdRp SARS-CoV-2
Antiviral drugs Lopinavir/Ritonavir HIV protease inhibitor HIV infection, SARS-CoV-1, and MERS-CoV
Antiviral drugs Darunavir/Cobicistat Protease inhibitor SARS-CoV-2
Antiviral drugs Favipiravir (T-705) Purine nucleotide RNA polymerase inhibitor RNA viruses and SARS-CoV-2
Antiviral drugs Ribavirin (Guanine analogue) Inhibits viral RdRp SARS-CoV-1 and SARS-CoV-2
Antiviral drugs Umifenovir (Arbidol) Targeting the S protein/ACE2 and inhibits the membrane fusion of the envelope of the virus Influenza and SARS-CoV-2
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Antimalarial drugs Chloroquine ( Synthetic version of quinine and is found in the bark of cinchona trees) Reduces the rate of replication Malaria, systemic inflammatory diseases, and SARS-CoV-2
Antimalarial drugs Hydroxychloroquine Inhibition of glycosylation of host receptors, proteolytic processing, and acidification of endosomes SARS-CoV-2 and autoimmune diseases
Antiparasitic drugs Ivermectin Inhibits nuclear transport Parasitic Infections and SARS-CoV-2
Antiparasitic drugs Nitazoxanide (Anti-helminthic drug) Unclear MERS and SARS-CoV-2
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Adjunctive drugs Corticosteroids/quinolone (n combination) Prevents ARDS SARS-CoV and SARS-CoV-2
Adjunctive drugs Monoclonal Antibodies (Tocilizumab, Sarilumab, Eculizumab, Fingolimod, Bevacizumab) Immunomodulatory effect, inhibition of terminal complement, and antiVEGF medication SARS-CoV-2 and Chronic Inflammatory disorders
Adjunctive drugs ACE-Inhibitors and ARBs ( enzyme ) Activates RAAS mechanism SARS-CoV-2
Adjunctive drugs Interferon-(a and ß) Unclear MERS-CoV and SARS-CoV-2
Adjunctive drugs Vitamin-D (Adjunct with vitamin C and zinc) Inhibits inflammatory response and attenuates cytokine storm SARS-CoV-2
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14.0 Vaccines

There are four categories of vaccines in clinical
trials
Whole Virus Vaccines- use a weakened
(attenuated) or deactivated form of the pathogen
that causes a disease to trigger protective
immunity to it.
Nucleic Acid Vaccines- use genetic material (DNA
or RNA) from a disease-causing virus or bacterium
(a pathogen) to stimulate an immune response
against it
Viral Vector Vaccines- use a modified virus (the
vector) to deliver genetic code for antigen into
human cells, thus infecting cells and
instructing them to make large amounts of
antigen, which then trigger an immune response.
Protein Subunit Vaccines- use fragments of
protein from the disease-causing virus to trigger
protective immunity against it.
Below is a list of authorized/approved vaccines
against SARS-CoV-2 for COVID-19 ( FDA Approved,
Emergency Use Authorization (EUA) vaccines)

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S/No Vaccine Name Vaccine Type Developers Country of Origin Current Schedule and Route of Administration Reported Effectiveness Following Clinical Trial
1. Comirnaty (formerly BNT162b2) mRNA-based vaccine(encodes mutated form of S protein) Pfizer, BioNTech Fosun Pharma Multinational Two doses, 21 days apart, intramuscular injection 95 efficacy in Phase 3 clinical trial (NCT04368728). 92 efficacy in vaccinated healthcare workers .
2 Moderna COVID-19 Vaccine ( mRNA -1273) mRNA-based vaccine Moderna, BARDA, NIAID USA Two doses, 28 days apart, intramuscular injection 94.1 efficacy in Phase 3 clinical trial (NCT04470427) .
3 COVID-19 Vaccine Janssen (JNJ-78436735 Ad26. COV2.S) Non-replicating viral vector Janssen vaccines (Johnsons Johnsons) The Netherlands, US Single dose vaccine, intramuscular injection 85 efficacy in Phase 3 ENSEMBLE trial (NCT04505722).
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4 COVID-19 Vaccine AstraZeneca (Covishield) Adenovirus vaccine BARDA, OWS UK Two doses, between 412 weeks apart, intramuscular injection 79 efficacy in Phase 3 clinical trial (NCT04516746). 100 efficacy in severe disease and hospitalization patients.
5 Sputnik V (Gam-COVIDVac) Recombinant adenovirus vaccine ( rAd 26 and rAd5) Gamaleya Research Institute, Acellena Contract Drug Research and development Russia Two doses, 21 days apart, intramuscular injection 94.1 efficacy in Phase 3 clinical trial (NCT04530396)
6 CoronaVac (formerly PiCoVacc) Inactivated vaccine ( formalin with alum adjuvant) Sinovac China Two doses, between 1418 days apart, intramuscular 50 efficacy in Phase 3 clinical trial (NCT04456595) .
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7 BBIBP-CorV Inactivated SARS-CoV-2 vaccine (Vero cell) Beijing Institute of Biological Products China National Pharmaceutical Group (Sinopharm) China Two doses, intramuscular injection 86 efficiency Phase 3 clinical trial ( ChiCTR 2000034780). High effectiveness in terms of neutralizing antibody production in rhesus macaques.
8 EpiVacCorona Peptide vaccine Federal Budgetary Research Institution State Research Center of Virology and Biotechnology Russia Two doses, 2128 days apart, intramuscular injection Phase1/2 trial (NCT04527575) Trial is still going and evaluation regarding efficiency being carried out.
9 Convidicea (Ad5-nCoV) Recombinant vaccine (adenovirus type 5 vector) CanSino Biologics China Single dose vaccine, but also evaluated in trial with 2- doses, intramuscular 65.7 efficiency in Phase 3 clinical trial (NCT04526990).
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10 Covaxin Inactivated vaccine Bharat Biotech in collaboration with National Institute of Virology), ICMR. India Two doses, intradermally 81 in Interim phase 3 trial
11 Name is yet to be specified Inactivated vaccine Sinopharm and the Wuhan Institute of Virology under the Chinese Academy of Sciences China Final number of doses and interval not yet decided Phase1/2 clinical trial (ChiCTR2000031809) is completed and 72.51 efficacy in on-going phase 3 clinical trial.
12 CoviVac Inactivated vaccine Chumakov Federal Scientific Center for Research and Development of immune and Biological Products Russia Not yet finally decided Phase1/2 trial is undergoing
13 ZF2001 Recombinant vaccine (CHO) Anhui Zhifei Longcom Biopharma ceutical, Institute of Microbiology of the Chinese Academy of Sciences China, Uzbekistan Not yet finally decided, intramuscular injection Phase 3 clinical trial (NCT04646590) is being evaluated.
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15.0 Control/Prevention

To prevent infection and to slow transmission of
COVID-19, do the following
Get vaccinated when a vaccine is available to
you.
Stay at least 1 metre apart from others, even if
they dont appear to be sick.
Wear a properly fitted mask when physical
distancing is not possible or when in poorly
ventilated settings.
Choose open, well-ventilated spaces over closed
ones. Open a window if indoors.
Wash your hands regularly with soap and water or
clean them with alcohol-based hand rub.
Cover your mouth and nose when coughing or
sneezing.
If you feel unwell, stay home and self-isolate
until you recover.

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16.0 Comparison of SARS-CoV2, SARS-CoV , and
MERS-Co
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17. References

https//www.who.int/emergencies/diseases/novel-cor
onavirus-2019
https//www.afro.who.int/health-topics/coronavirus
-covid-19
https//en.wikipedia.org/w/index.php?titleSevere_
acute_respiratory_syndrome_coronavirus_2oldid104
5920399
https//doi.org/10.1016/j.cell.2020.04.013
. Romano M, Ruggiero A, Squeglia F, Maga G,
Berisio R. A Structural View of SARS-CoV-2 RNA
Replication Machinery RNA Synthesis,
Proofreading and Final Capping. Cells.
202091267.
S. Raskin, Genetics of COVID-19, Jornal de
Pediatria, https//doi.org/10.1016/j.jped.2020.09.
002
Nanotechnology for Environmental Engineering
(2021) 619. https//doi.org/10.1007/s41204-021-00
109-0

Yadav, R. Chaudhary, J.K. Jain, N. Chaudhary,
P.K. Khanra, S. Dhamija, P. Sharma, A. Kumar,
A. Handu, S. Role of Structural and
Non-Structural Proteins and Therapeutic Targets
of SARS-CoV-2 for COVID-19. Cells 2021, 10, 821.
https//doi.org/10.3390/cells 10040821
https//doi.org/10.1371/journal.ppat.1008536.g003
Jha, N.K. Jeyaraman, M. Rachamalla, M. Ojha,
S. Dua, K. Chellappan, D.K. Muthu, S. Sharma,
A. Jha, S.K. Jain, R. et al. Current
Understanding of Novel Coronavirus Molecular
Pathogenesis, Diagnosis, and Treatment
Approaches. Immuno 2021, 1, 3066.
https//doi.org/ 10.3390/immuno1010004
https//en.wikipedia.org/w/index.php?titleSpecial
CiteThisPagepageInfluenza_pandemicid104212477
9wpFormIdentifiertitleform
https//upload.wikimedia.org/wikipedia/commons/thu
mb/b/b4/Symptoms_of_coronavirus_disease_2019_3.0.s
vg/800px-Symptoms_of_coronavirus_disease_2019_3.0.
svg.png
J Gene Med. 202123e3303. https//doi.org/10.1002
/jgm.3303
Audio https//youtu.be/Q2MmREArTds