Viruses Flashcards
What are virus exclusive polymerases?
RNA dependent RNA polymerase
RNA dependent DNA polymerase- reverse transcriptase
How do viruses get envelopes ?
Viruses that can exit an infected cell without destroying it
Viruses that exit via budding can leave the membrane intact
Enveloped viruses synthesis several classes of proteins that stud the membrane so it can continue infection
Name the seven viral groups
1- ds DNA viruses eg. HSV 2- ss DNA viruses eg. Parvovirus 3- ds RNA virus eg. Reovirus 4- (+) sense RNA virus eg HCV 5- (-) sense RNA virus- influenza 6- RNA reverse transcribing virus- HIV 7- RNA reverse transcribing virus- HBV
Describe the formation of virus particle envelopes
Mostly viral particles use the cellular membranes as site of assembly, could be the nuclear envelope, Golgi membrane or the plasma membrane
Matrix proteins- internal proteins that link the capsid to the envelope- usually glycosylated
Glycoproteins- external- anchored in the membrane by a transmembrane domain (sometimes 2)
-transport channel- contain several transmembrane domain forming a protein lined channel
Describe virus penetration
Fusion from within
pH dependent
Takes advantage of receptor recycling- escapes the endosome usually via acidification by viral protein pumps
Fusion from without
pH independent
Binding with a receptor that transports it across the membrane
Describe genome packaging
Eg. The helical plant virus TMV
The packaging signal (psi signal) in the viral genome allows the virus to differentiate between the genomic nuclei acids and cellular background
The origin of assembly sequence (OAS) in the nucleic acid binds to a disc protein that form rings encasing the nucleic acid
The front face condenses twice as fast as the back so the OAS is usually found 1/3 of the way through the nucleic acid
Describe the early events of virus invasion
Random collision with cell- initial electrostatic attraction because of opposite charge
Only binds if the cell has an appropriate receptor- enveloped viruses use their surface glycoproteins- determines tropism as the trimeric glycoproteins have affinities
Non-enveloped viruses use capsid proteins
Virus hijacks cell surface molecule to aid it’s entry
Some cell receptors have more than virus and some viruses use for than one receptor
What is the significance of heptad repeats?
Used by viruses eg. HIV when docking at the plasma membrane
Found on the virus envelope
Facilitate fusion from within and escape from the endosome
How do viruses get to their targeted compartments in the cell?
Uses localisation signals when travelling via the cytoskeleton
Eg. HIV uses the same localisation motif that histones uses to get to the nucleus- capsid is disassembled on binding with the nuclear pore and the DNA is imported in
How does tropism affect virus production?
Virus may be able to bind but not enter, enter but not replicate, replicate but not mature
Eg. Human influenza requires a specific protease found only in airway epithelial cells
Briefly describe HIV cell interactions and post entry processing
Trimeric viral spike contains gp120 that binds to CD4 and then the chemokine receptor CCR-5
Host cyclophilin A packaged by the virion is required for normal uncoating
If there is no cyclophilin- abortive reverse transcription
Describe the genome replication of class 4 viruses?
Single stranded +sense RNA
Transcription of protein can occur directly from the virion RNA after replication
Describe the genome replication of class 5 viruses
Single stranded -strand RNA that required replication before it can be transcribed- ha to make dsRNA intermediate
Describe the genome replication of class 3 viruses
Double strand RNA
Replication has to occur before transcription is known to occur in a partially dissembled virion
Describe the genome replication of class 6 viruses
Reverse transcribing RNA
Single strand +sense RNA with a DNA intermediate
Replication generates a DNA copy of the RNA which integrates into the host genome
Describe the genome replication of class 7 viruses
Reverse transcribing DNA viruses
DsDNA with an RNA intermediate
The cDNA copy of the virus is generated during exit not entry
Describe the genome replication of class 1 viruses
DsDNA
Virus has proteins- immediate early that switch proteins on
Early proteins are non-structural proteins that orchestrate the host
Late proteins- structural proteins
Happens in nucleus
Describe the genome replication of class 2 viruses
Single stranded DNA
SsDNA intermediate is packaged into virion and replication usually occurs before any transcription of protein
Describe vital entry strategies
Picornaviruses have many viruses that all utilise the sane receptors
Eg. 91 strains of the Rhinovirus all use ICAM1 so does coxsackie A
Ebola can use many different receptors as one virus eg. DC-SIGN, TREM, APC, asialoglycoprotein, TLR, NPC1- this means that it has many tropisms and an infect many types of cells
Hepatitis C binds to many receptors in sequence which process tropism for liver cells SR-B1➡️ CD81➡️ CLDN1➡️ occludin➡️ entry
What is the significance of eIF-4G in VEHCS?
Component of the eLF-4F cap binding complex which acts as a bridge between the eLF-4E cap structure and the 40S subunit if the ribosome
Cleavage eIF-4G by VP2A inactivated cap-dependent translation with eLF-4A
Then the internal ribosome entry site (IRES) of the poliovirus can directly recruit 40S TK the viral RNA and initiate cap-independent translation
What other methods are involved in VEHCS and eIF-4G?
DNA and -RNA viruses dephosphorylate eIF-4E do it does not bind to eIF-4G
+RNA viruses dephosphorylate eIF-4Ebp so eIF-4E cannot bind to eIF-4E
Rotaviruses make a eIF-4G binding protein, nsP3, which makes the cap complex eject the host RNA by displacing the poly-A bp Pab1b allowing the virus RNA to bind nsP3 and populate the initiation complex
The influenza virus inserts viral transcript into the open reading frame of host RNA transcripts
Describe the genome structure of +ssRNA viruses
Linear
Cassette organisation of structural proteins and non structural proteins
Usually 5’ methyl caps and polyA tails (except picornavirus has Vpg cap and flavivirus doesn’t have polyA tail)
Usually 5’ and 3’ UTRs )except coronavirus)
Describe the genome structure of -ve sense RNA viruses
Can be simple or complex
Simple- rhabdoviruses contains many starts, stops and polyAs, paramyxovirus contains pause signal to effect ribosome shuttling and arenaviruses ambisense
Multipartite viruses have segmented genomes that are packaged into multiple particles eg orthomyxovirus
Filovirus eg Ebola initiations of some proteins can overlap with others
Describe herpesviruses
Subfamilies of alpha, beta and gamma
Alpha- herpes simplex virus 1 and 2 (HSV1,2) and varicella-zoster virus (VZV)
Beta- cytomegalovirus (CMV), human herpes virus 6 and 7 (HHV6,7)
Gamma- Epstein Barr virus (EBV), Kaposi’s sarcoma-associated herpesvirus (KSHV)
Enveloped with a icosadeltahedral capsid
Linear dsDNA- replicate in the nucleus
Glycoproteins embedded in lipid envelope for receptor mediated entry
Tegument between envelope and capsid that induces viral gene expression and VEHCS and virus assembly
Describe the human herpes viruses
Alpha- HSV1,2 (mucoepithelial cells) and VZV (B cell, epithelial cells) variable host range, short replication cycle, rapid spread in culture and efficient destruction of infected cells
Beta- CMV (epithelial cells, monocytes, lymphocytes), HHV6,7 (T lymphocytes) restricted host range, long replication cycle, slow spread
Gamma- EBV (B cells, epithelial cells), KSHV (B cells, endothelial) restricted host range, usually specific for lymphocytes, latent infection in lymphocytes, relocation in culture is infrequent
They can be latent (no virus protein expression, immunologically silent, episomal DNA replicated with host DNA) or lytic (virus DNA replication, new progeny viruses made, virus protein expressed, highly immunogenic)
Describe herpesvirus binding and entry into the host
Conserved glycoproteins
Glycoproteins B, H, L, M, N
Receptor mediated endocytosis or direct fusion with the plasma membrane
Describe a herpes virus life cycle
- Viral DNA circularisation
- Expression of immediate early genes to transactivate viral DNA replication and inhibits host promoters
- Expression of early genes- viral replication
- Expression of late genes- structural genes
- Production of viral capsid, tegument, glycoproteins
- Production of viral progeny- PM makes the virus envelope
Describe herpesvirus DNA replication
They encode their own proteins for viral DNA replication- ssDNA binding protein, origin binding protein, helicase-primase complex, DNA polymerase, polymerase prices diving factor
1. Input DNA is circularised upon entry to the cell
2. Origin binding protein binds to specific sequences within the origin of replication
3. The origin binding proteins begin to unwind the DNA
4. The unwinding DNA forms a replication bubble
5. The origin binding protein begins to recruit ssDNA binding proteins
6. The origin binding proteins and ssDNA binding proteins to the replication forks
DNA is nicked during replication to form a rolling circle
Describe the clinical manifestations of herpes simplex infections
Infection via mucosal surfaces
Replication in oral or genital mucosa
Invasions via sensory endings
Neurovirulence- invade and replicate in the CNS, severe neurological devastation
Latency- HSV1 in the trigeminal ganglion
HSV2 in the sacral ganglia
Severity directly related to type of immunosuppressive therapy used after a transplant
More exaggerated, frequent and anti-viral resistant in HIV/AIDS