Exam 2 - Lecture 5 Flashcards
What is the “purpose” of viral replication (from the virus perspective) and why should we care about it?
The purpose of viral replication is for the virus to make more of itself and further infect a host cell
Viral replication leads to cell death and human disease, and viral treatments are almost always virus-specific, so it’s important to understand how viruses replicate
Attachment
- What types of chemical bonds are used?
Noncovalent bonds (H bond, van der Waals, ionic)
Attachment
- Know the general names of the proteins that interact (on virus and host cell), how specific the interactions are, and the concept of multi-step attachment
There are host cell receptors that interact with adhesins (adhesion proteins) on the virions
- these interactions are extremely specific in the tissue tropism and host range
Some viruses can use different receptors to infect different cell types (primary receptor and co-receptor); some viruses may use alternative receptors if the primary receptor is not available
Attachment
- What is meant by tissue tropism and host range?
Tissue tropism: tissue type infected by the host
Host range: species infected by the virus
Attachment
- Know the experiments that can be done to prove that a host protein is serving as a receptor
1) add an antibody specific for the suspected receptor and see if viral attachment is blocked
2) add extra amounts of the normal ligand for the receptor and see if viral attachment is blocked
3) add the receptor to a viral-resistant cell and see if the virus attaches
4) add a soluble form of the receptor and see if the virus attaches
Attachment
- What are the different classes of host proteins/products used as receptors by viruses?
1) cell adhesion receptors
2) cytokine and growth factor receptors
3) glycoproteins containing sialic acid
4) bacterial products
Attachment
- What specialized parts of cell membranes often contain high levels of receptors (for viruses)?
Lipid rafts, intracellular joints, and clathrin-coated pits
What cellular/viral changes occur when adhesins bind to receptors?
Understand the concept of permissiveness (and its relationship to attachment)
1) binding often triggers a conformational change in the adhesin and receptor
2) changes to the receptor can trigger clathrin recruitment to the membrane
3) binding can activate signal transduction in the host cell
How do some viruses access particularly challenging cell membranes (what strategies do they use?)
1) wait for damage to the tissue
2) encode an enzyme to help break through the barriers
3) physical force through using an injectisome
Where are viral adhesins located on naked vs enveloped viruses?
Naked: on capsid in pockets, on the outer surface of the capsid, or on protruding spikes
Envelope: embedded in the envelope
What is meant by entry?
viral entry: crossing the plasma membrane and gaining access to the cytosol
Plasma membrane entry
- Know the mechanism by which naked viruses enter at the plasma membrane
- Same for enveloped viruses…what are fusion proteins and how do they work?
Naked viruses: enter the PM by directly injecting the genome through a pore created in the bilayer
Enveloped viruses: can fuse their envelope directly with the plasma membrane
- Fusion proteins in the viral envelope help pull the two membranes together
Internal membrane entry
- How do the virions get into an endosome?
- What is special about endosomes that aids in viral entry? (what is inside of those endosomes)
Instead of entering directly into the cytosol, virions trigger an endocytosis event and are brought into an endosome as a result of attaching to the PM
pH of the endosome becomes acidic and allows for viral entry
Internal membrane entry
- What are advantages to entering via internal membranes?
1) make it through the plasma membrane cortex
2) can use endosomal tracking to move more easily deep into the cytosol
3) better at hiding from the immune system
Uncoating
- What is it and what are some mechanisms that are used?
Uncoating: the genome escapes the protein capsid shell
Mechanisms
- Some uncoat during entry at the PM, others in the endosome
- Some uncoat due to cytosolic enzymes degrading it
- Some relatively intact capsids expel the genome
