100% tevredenheidsgarantie Direct beschikbaar na betaling Zowel online als in PDF Je zit nergens aan vast
logo-home
Eerder door jou gezocht
Eerder door jou gezocht
logo
Summary Virology €7,99   In winkelwagen
Snel navigeren naar
Voorbeeld
  2.  
  3. Universiteit Antwerpen (UA)
  4.  
  5. Biochemie En Biotechnologie
  6.  
  7. Virology

Samenvatting

Summary Virology
 73 keer bekeken  2 keer verkocht

Resume of the theory given in the lessons of Virology. In case figures from handbooks were used, information of the handbook is also added!

Voorbeeld 4 van de 44  pagina's

Document informatie

  • 16 mei 2023
  • 44
  • 2021/2022
  • Samenvatting

Onderwerpen

Geschreven voor

Alle documenten voor dit vak (1)

Verkoper

avatar-seller
studentua99

Ontvangen beoordelingen

Voorbeeld van de inhoud

AN INTRODUCTION TO VIROLOGY
WHAT ARE VIRUSES
Viruses are the smallest, simplest & most abundant form of life on Earth
 Can infect all forms of life (plants, animals, eukaryotes, bacteria)
 Virion: complete, infectious virus particle
 Genetic material: DNA or RNA, ss or ds
o Enclosed in protein coat (= capsid)
 Sometimes lipid membrane (= envelope)
 Viral genome:
o 2 core modules
 Structural proteins  Virion formation (building blocks)
 Non-structural proteins  Genome replication
o Encode for:
 Capsid protein
 Receptor-binding protein
 Viral polymerase
o Doesn’t encode for:
 Protein synthesis machinery
 Proteins for membrane synthesis
 No centromeres or telomeres in standard host chromosomes
 Diameter: 20 – 500 nm
 High abundance, but low relative biomass
 Visualizing: electron microscope

Viruses are obligatory parasites (= can only function after replication in a host cell)
 Depend on host cell for:
 Energy production:
o Mostly ATP, by photosynthesis or metabolism of sugars..
 Protein synthesis
o Ribosomes, transfer RNAs, specific enzymes
o Host ribosomes translate mRNA made by virus
 Reproduction
o Host cell provides building blocks
 Revolution

Viruses are important disease-causing agents
 HIV, Hepatitis, Influenza…
 !!! Not all viruses make us sick
 Most are passengers through our body
 Immune system deals w/ (some) viruses

Viruses have high genome evolution rates
 Evolve rapidly
 Higher mutation rate than eukaryotes & bacteria
 Corona virus has largest RNA genome as we
known for so far

Viruses must be excluded from the tree of life, because:
 Not alive
 No ancestral viral lineages
 No structure derived from a common ancestor




1

,ORIGIN OF VIRUSES
Primordial virus world or viral early hypothesis
= viruses are direct descendants of the first replicons that existed
during the pre-cellular stage of the evolution of life
 Viruses existed before cells
 Go very far in evolution, are very ancient

Reductive virus origin
= viruses are the ultimate products of degeneration of ancestral cells
that lost their autonomy & transitioned to obligate intracellular parasitism
 Cells before viruses

Escaped genes hypothesis
= viruses evolved on multiple, independent occasions in different cellular
organisms from host genes that acquired the capacity for autonomous,
selfish replication and infectivity
 Specific genes split off in particles and evolve to viruses

CLASSIFICATION OF VIRUSES: BALTIMORE CLASSIFICATION



Based on the following principles:
 Nature, strandedness, orientation
& topology of nucleic acids
 Nucleotide sequence
 Symmetry of the capsid
 Presence of an envelope
 Virion & capsid dimensions




DNA GENOMES VERSUS RNA GENOMES

DNA genomes RNA genomes
 Genetic material is based on DNA  Genetic material is based on RNA
 Most replicate in the nucleus  A lot of diversity:
 Use host’s DNA- & RNA-synthesizing + RNA-processing  ss or ds
machinery  (+) or (-)
 Dominant in prokaryotes  Linear of segmented
 Classes 1 & 2 of Baltimore system  Most replicate in cytoplasm
 Genome have to encode RNA-dependent RNA
polymerase (RdRp) (cells don’t have this)
 Produces RNA genomes & mRNA from RNA
templates
 Dominant in eukaryotes
 Classes III – VII in Baltimore system




2

,CLASSES OF BALTIMORE CLASSIFICATION

Class Features Examples Replication
I  Wide variety in genome size  Adenovirus  Nucleus
(gapped) dsDNA
 Have unfragmented genomes  Herpes virus  DNA  DNA
genomes
 Circular or linear DNA
 No infection of plants
II  Very small & have few genes  Parvovirus  Nucleus
ssDNA genomes
 Replication in nucleus  DNA  DNA
 Circular genomes (dsDNA
 Specific enzyme holding intermediate)
III  Mostly fragmented  Rotavirus A  Cytoplasm
dsRNA genomes
 1 gene encodes for 1  RNA  RNA
protein
 All have icosahedral capsid
symmetry
IV  Most plant & many  Corona virus  Cytoplasm
ss(+)RNA genomes
vertebrate viruses  Yellow fever virus  (+)RNA  (-)RNA
 All linear genomes  Poliovirus
 Small: non-  Hepatitis A virus
enveloped
 Larger: enveloped
 Larger & many plant RNA
viruses have helical capsids
V  Helical nucleocapsids  Ebola virus  Cytoplasm/nucleus
ss(-)RNA genomes
 Some are fragmented  Rabies virus  RNA  RNA
 Not found yet in prokaryotes  Influenza A virus
 Linked to the most  Measles virus
widespread & deadly diseases
VI  Integrated parts of dsDNA in  HIV  Cytoplasm
ss(+)RNA genomes w/
genome of host  RNA  DNA
DNA intermediate
VII  Not originally identified by  Hepatitis B virus  Nucleus &
dsDNA genomes w/ RNA
Baltimore cytoplasm
intermediate
 Gapped dsDNA genomes  DNA  RNA and
 Gaps are filled by then RNA  DNA
reverse transcriptase
& genome is copied
into RNA
intermediate

THE VIROLOGY TOOLBOX
STEP 1: VIRUS ISOLATION & PROPAGATION

 Susceptible cell: functional receptor  may or may not be competent to support viral replication
 Resistant cell: no functional receptor  “
 Permissive cell: capacity to replicate virus  may or may not be susceptible
 Susceptible & permissive cell: can take up & replicate the virus particle for sure

Infection of cells depends on the random collision of virus particles w/ cells
 not all susceptible cells are infected when virus is added

!!! Not all virus particles are infectious
 particle-to-PFU ratio = (# physical viral particles)/(# infectious viral particles)

Multiplicity of infection (MOI): the number of infectious particles added per cell
 MOI = PFU/(number of cells)
 Example: MOI = 10  adding 107 virus particles per 106 cells



STEP 2: VIRUS DETERMINATION
3

, PLAQUE ASSAY (QUANTITIVE)
Method:
1. Inoculation of bacteria on nutrient agar in Petri dish
2. Dilutions of a phage suspension
(virus stock, concentration unknown)
3. Add 0,1 ml of dilution to Petri dish
4. Count lysis area = plaque
o Phage binds to bacterial cell
 cell releases progeny phage particles
 taken up by neighboring cells + replicated
 lysis of the cells in a circular area surrounding the original infected cell
 1 plaque = 1 infectious virus particle

HEMAGGLUTINATION (PHYSICAL)
Principle: sialic acid receptors on red blood cells bind to hemagglutinin glycoproteins found on the surface of several viruses
 Advantages:
 Simple
 Inexpensive
 Limitations:
 Controlling incubation times
 RBC type & virus concentration
 Interfering factors in the sample
(pH, T, buffer composition)
 Qualified personal required

ELECTRON MICROSCOPY (PHYSICAL)
 Most recently: cryo-EM

VIRAL ENZYME ACTIVITY (PHYSICAL)
Principle:
 Reverse transcriptase (RT) is used
to synthesize a labeled DNA strand
 DNA labeling can be done w/ radiolabeled
or fluorescently labeled nucleotides
 Labeled DNA can be quantified & the amount
is proportional to the RT activity in the sample

SEROLOGY (PHYSICAL)
= Indirect Immuno Fluorescense Test

 Direct: viral antigen/protein detection
 Indirect: antiviral antibody detection

NUCLEIC ACID DETECTION (PHYSICAL)
= viral genome detection by PCR

VIRUS STRUCTURES
From big to small:
 Virion: infectious virus particle
 Envelope: lipid bilayer derived from host cell (sometimes)
 Nucleocapsid: protein/nucleic acid aggregates within the capsid
 Capsid: protein shell surrounding the genome
 Structural unit: unit from which (nucleo)capsids are build, can contain >1 subunits
 Subunit: single folded polypeptide chain

Functions of structural proteins:
 Protection fragile viral genome
4

Voordelen van het kopen van samenvattingen bij Stuvia op een rij:

√ Verzekerd van kwaliteit door reviews

√ Verzekerd van kwaliteit door reviews

Stuvia-klanten hebben meer dan 700.000 samenvattingen beoordeeld. Zo weet je zeker dat je de beste documenten koopt!

Snel en makkelijk kopen

Snel en makkelijk kopen

Je betaalt supersnel en eenmalig met iDeal, Bancontact of creditcard voor de samenvatting. Zonder lidmaatschap.

Focus op de essentie

Focus op de essentie

Samenvattingen worden geschreven voor en door anderen. Daarom zijn de samenvattingen altijd betrouwbaar en actueel. Zo kom je snel tot de kern!

Veelgestelde vragen

Wat krijg ik als ik dit document koop?

Je krijgt een PDF, die direct beschikbaar is na je aankoop. Het gekochte document is altijd, overal en oneindig toegankelijk via je profiel.

Tevredenheidsgarantie: hoe werkt dat?

Onze tevredenheidsgarantie zorgt ervoor dat je altijd een studiedocument vindt dat goed bij je past. Je vult een formulier in en onze klantenservice regelt de rest.

Van wie koop ik deze samenvatting?

Stuvia is een marktplaats, je koop dit document dus niet van ons, maar van verkoper studentua99. Stuvia faciliteert de betaling aan de verkoper.

Zit ik meteen vast aan een abonnement?

Nee, je koopt alleen deze samenvatting voor €7,99. Je zit daarna nergens aan vast.

Is Stuvia te vertrouwen?

4,6 sterren op Google & Trustpilot (+1000 reviews)

Afgelopen 30 dagen zijn er 67474 samenvattingen verkocht

Opgericht in 2010, al 14 jaar dé plek om samenvattingen te kopen

Start met verkopen
€7,99  2x  verkocht
  • (0)
  Kopen