Influenzaviruses

Question 1

What family do influenzaviruses belong to? How many strains are there?

Answer 1

Orthomyxoviridae family

3 Types of Influenza: A, B and C

• Within each type there are multiple subtypes
• All 3 can infect and cause symptoms in humans, but pandemics caused solely by Type A
• Infection with one type or subtype does not confer immunity to another type of influenza

Question 2

Which type of influenza is the cause of of major outbreaks throughout history?

Answer 2

Influenza Type A

Question 3

What is the following of Influenza Type A:

• Host Range
• Epidemiology
• Clinical Features
• Genome
• Structure

Answer 3

• Host Range: Humans, pigs, horses, birds,
• Epidemiology: Antigenic Shift and Drift
• Clinical Features: May cause pandemics (esp. young ppl)
• Genome: 8 gene segments
• Structure: 10 viral proteins & M2 unique

Question 4

What is the following of Influenza Type B:

• Host Range
• Epidemiology
• Clinical Features
• Genome
• Structure

Answer 4

• Host Range: Humans only
• Epidemiology: Antigenic Drift only
• Clinical Features: Severe Disease; elderly, no pandemic
• Genome: 8 Gene Segments
• Structure: 11 viral proteins

Question 5

What is the following of Influenza Type C:

• Host Range
• Epidemiology
• Clinical Features
• Genome
• Structure

Answer 5

• Host Range: Humans and Pigs
• Epidemiology: Antigenic Drift only
• Clinical Features: Mild disease, common in children
• Genome: 7 Gene Segments
• Structure: 9 viral proteins

Question 6

What is Antigenic Shift?

Answer 6

hemaglutinnin protein

cell gets infected by two strains

the two strains can mix/match their RNA genomes called reassortment

produces hybrid viruses that ppl most likely don’t have immunity for

Question 7

What is Antigenic Drift?

Answer 7

subtle changes/mutations in the hemaglutinin proteins

changes a little bit as it replicates

Question 8

What is the difference between antigenic shift and drift?

Answer 8

Shift = etnirely new hemaglutinin  (more dramatic = major change)
Drift = subtle changes; slight mutation to hemaglutinin protein

Question 9

How is virus nomenclature used to name viruses?

Answer 9

Influenza type (genus)
Species isolated form (unless human)
Place of Isolation
Number of the isolate
Year of isolation
H and N subtypes (18 H and 11 N subtypes)

Question 10

How would you name the 220th isolate of an H5N1 subtype virus isolated from chickens in Hong Kong is designated?

Answer 10

A/chicken/Hong Kong/220/97(H5N1)

Question 11

What makes up the virion structure of influenzaviruses?

Answer 11

Envelope contains the H and N glycoproteins and M2 protein

Ribonucleoprotein complex (RNPs) make up the core of the virus. RNPs consist of

• viral RNAs complexed with the polymerase proteins
• PB1, PB2 and PA code for RDRP

Question 12

How does influenza virus infect its host? (Attatchment/entry, uncoating, replication)

Answer 12

HA attaches virion to sialic acid residues on surface of host cell

virus enters through endocytosis

progressive acidifcation of endosome

• M2 ion channel allows protons into core of virus =
• Acidification = conformational change of hemaglutinin
• pokes hole in endosome
• allows release viral RNA segments
• endonucleus guides viral segments to nucleus

When viral RNA segments get into the host nucleus:

• (-) RNA segments have to be transcribed to (+) RNA -
• (RDRP = PB1, PB2, PA segments)
• cell ribosomes can recognize the (+) RNA and produce viral proteins

Question 13

What are the functions of the following influenzavirus proteins that make up the ribonucleoprotein complex?

Answer 13

PB1, PB2, PA = RNA Dependent RNA Polymerase

HA = Hemaglutinin binds sialic acid residues on surface of host cell for attachment

NA = Neuraminidase cleaves sialic acid residues on surface of host cell for exit of new virions

M2 = ion channel that allows protons to enter virion and causes conformational change to hemaglutinin that results in release of viral segments into host cytoplasm

Question 14

What is the influenzavirus lifecycle?

Answer 14

1. Attachment to sialic acid
2. Endocytic entry
3. Uncoating and release of vRNPs into cytoplasm
4. Translocation of vRNPs into nucleus
5. Generation of mRNA and positive (+) strands and more (–) strand RNA genomes
6. Production of viral proteins
7. Genomes packaged into pre-assembled capsids
8. Budding and release of progeny virions

Question 15

What are the characteristics that influence influenzavirus attachment?

Answer 15

Hemagglutinin Binding to sialic acid linked to galactose on cell surface

Human viruses bind α2,6 Galactose (in respiratory tract)

Avian viruses bind α2,3 Galactose (in bird intestines)

Difference influences pathogenesis in these two species

Question 16

What change in binding specificity made the spanish flu so deadly?

Answer 16

Current work suggests that a single amino acid change within the HA of Spanish flu (1918 pandemic) resulted in the ability of this avian flu virus to now bind α2,6 Galactose

Normal avian viruses bind α2,3 Galactose

Question 17

Go over the uncoating step for influenzaviruses.

Answer 17

M2 ion channel in the viral envelope allows H+ ions to penetrate the virion

Weakens the viral M1 matrix protein from the vRNPs

vRNPs released into the cytoplasm

Question 18

What drugs block the uncoating step in influenzaviruses?

Answer 18

Amantidine (sold as Symmetrel) and rimantidine (sold as Flumadine) block the M2 ion channel function, interfering with uncoating.

Question 19

What do influenzaviruses have to do in order to replicate? What about making viral proteins?

Answer 19

Replication

• have to make (+) RNA antigenome
• template to make more (-) ssRNA influenzaviruses

Viral Proteins
- (+) RNA antigenome is used to translate viral proteins using host ribosomes

Question 20

How are influenza virions released from host cell?

Answer 20

Virions are released by budding

The viral NA protein cleaves the sialic acid on host cells to prevent clumping of viral particles at the host surface.

Question 21

What drugs interrupt virion release of influenza viruses?

Answer 21

Zamanivir (sold as Relenza) and oseltamivir phosphate (sold as Tamiflu) inhibit the function of NA.

Question 22

Go over the pathogenesis of influenzaviruses.

Answer 22

droplet transmission

Virus enters respiratory tract

Attaches to ciliated columnar epithelial cells lining the sinuses and airways

Primary site of infection—tracheobronchial tree, involving nasopharynx

As virus replicates, cilia are destroyed

• Cleaning system in the lungs does not work as well
• mucus stays in the airway causing coughing
• Virus replication peaks at 48 hours and then declines
• Virus shed for up to a week

Destruction of cilia contribute to secondary bacterial pneumonia infections, sinusitis, otitis

Question 23

What is the incubation period for influenza? Who are the carriers? How is it transmitted?

Answer 23

Influenza has a short INCUBATION PERIOD within the host

• Infection to symptoms is approximately 1 to 2 days

Infected individuals act as ACUTE CARRIERS of the disease

Infected individuals readily TRANSMIT the virus by coming
into contact with un-infected individuals or by expelling the virus into the environment in the form of FOMITES

Question 24

What are the clinical features of an uncomplicated infection from influenza?

Answer 24

Onset of symptoms:
Headache
Aching in the limbs and back
Fever (100-103oF)
Malaise
Dry cough
Sore throat
Chest X-ray is normal

Usually resolves itself after 7 days

Question 25

What are the clinical features of an complicated infection from influenza?

Answer 25

Age-dependent

Young children—croup, secondary bacterial pneumonia, middle ear infections

Elderly—life threatening secondary bacterial pneumonia, pre-existing conditions like congestive heart disease exacerbated

Immune compromised individuals—at risk of death during an influenza epidemic

Question 26

How do you develop immunity for influenzaviruses?

Answer 26

Infected individuals develop antibodies against the outer proteins of Influenza virus—neuraminidase (NA) and hemagglutinin (HA)

Antibodies against HA neutralize the virus

Antibodies against NA do not but they do reduce the release of virus from infected cells

Question 27

What composes the trivalent influenza vaccine?

Answer 27

Recommendations made based on antigenic analyses of recently isolated influenza viruses, epidemiologic data and post-vaccination serologic studies in humans

Vaccine is a cocktail of 3 virus strains

• 2 strains of Influenza A
• 1 Influenza B strain

Question 28

What determines effectiveness of influenza vaccine?

Answer 28

Age of the vaccine recipient

Immunocompetence of the recipient

Degree of similarity between the viruses in the vaccine and those in circulation

Question 29

What are the antivirals used for influenza?

Answer 29

First drugs: M2 inhibitors (prevent uncoating step)

• Amantidine (sold as Symmetrel)
• Rimantidine (sold as Flumadine)

New class of antivirals: NA inhibitors (prevents neuraminidase from cleaving sialic acid during budding)

• Cause viruses to clump at cell surface, reduce viral spread
• Oseltamivir (sold as Tamiflu, pill form)
• Zanamivir (sold as Relenza, must be inhaled)

Question 30

What is the mechanism for generation of new pandemic influenza Type A viruses?

Answer 30

Reassortment

Question 31

What was significant about the mortality rates for the spanish flu when compared to regular flu?

Answer 31

Spanish flu had a W shaped mortality curve instead of a U shaped curve

Killed 20-40 y/o’s more than regular flu

Question 32

What were the researchers trying to accomplish in this study? What was their hypothesis? What were their goals?

BIRD FLU PAPER

Answer 32

Find out what changes need to occur to this bird flu strain to make easier to transmit from person to person (possible pandemic).

This bird flu is highly virulent but low transmissibility. Is it possible to mutate virus so that it can spread via aerosol route. Thought they could mutate it by changing the HA.

Question 33

How did the researchers carry out their study? What methods did they employ to accomplish their research objectives.

BIRD FLU PAPER

Answer 33

First made changes in viral protein that binds receptor (hemaglutinin - sialic acid).
- Thought this would increase transmissibility b/c they wanted to change it from alpha-2-3 sialic acid (binds birds better) to alpha-2-6 sialic acid (binds humans easier)

Initial change did not make it more transmissible.

Second, they serially passaged the virus through ferrets (infect 1 group, take out infect 2nd group etc) to allow the virus to evolve with each replication. Hoping to see mutations as result of viral replication.

Question 34

Why did they choose the A/Indonesia/5/2005 (H5N1) strain for this study?

BIRD FLU PAPER

Answer 34

highly virulent. incidence of human A/H5N1 virus infections and fatalities in Indonesia remains fairly high

concerns this virus could mutate to increase transmissibility between humans and cause a pandemic.

Question 35

Why did they choose ferrets as their animal model?

BIRD FLU PAPER

Answer 35

Susceptible to infection with human and avian influenza viruses

Develop respiratory disease and lung pathology similar to that observed in humans

Ferrets can also transmit human influenza viruses to other ferrets that serve as sentinels with or without direct contact.

Question 36

Describe the main findings of the paper.

BIRD FLU PAPER

Answer 36

After passaging virus 10 times they noticed they had 4 mutations to HA in addition to their original change they did themselves
- The other mutation was on PB2 (one of the genes needed for RDRP)

They observed that the virus could become airborne transmissible

Also the mutations that brought on airborne transmission also mutated the virus to become less virulent too.

Question 37

What are some of the scientific and societal implications of this work?

BIRD FLU PAPER

Answer 37

The mutations that arose in this SINGLE strain arose through antigenic drift (usually pandemics arise through antigenic shift) so you can get pandemic strains through antigenic drift too.