Effector Immunity- viruses, bacteria, parasites

Question 1

What type of effector response is needed?

Answer 1

Depends on the type of pathogen and the danger signals that are being detected by the innate immune system

Question 2

Immune response for intracellular pathogens

Answer 2

• Th1 type
• Leads to cytotoxic T cells, IFN-gamma, NK cells

Question 3

Immune response for extracellular pathogens

Answer 3

• Th2 type
• Leads to antibody response

Question 4

Immune response for extracellular at mucosal surfaces

Answer 4

• Th17 type
• Leads to IL-17, IL-23, regulators of mucosal responses, tolerance
• Can lead to autoimmune disease if response fails

Question 5

Immune response to no danger signals (non-dangers)

Answer 5

• Ex. foods, environmental
• T regulatory response

Question 6

What is an intracellular pathogen?

Answer 6

• Viruses
• Bacteria
• Parasites

Question 7

What is an extracellular pathogen?

Answer 7

• Bacteria
• Parasites
• Fungi

Question 8

Viruses

Answer 8

• Intracellular pathogens. Basically proteins with some glycogen residues and a genome
• Require cell machinery for replication (injects RNA or DNA into host cell for replication)
• Have no metabolism
• Lead to Th1 response and cytotoxic T cells

Question 9

Viruses and evolution

Answer 9

• Often share a close evolutionary relationship with their hosts. A symbiotic relationship would be best but not always possible

Ex. retroviral integration into the genome (HIV and SIV)

Question 10

Virus shape and size

Answer 10

• Highly organized but simple structure
• Can be naked or enveloped
• Small, 20-400nm

Question 11

Smallest virus

Answer 11

Rhinovirus

Question 12

Largest virus

Answer 12

smallpox

Question 13

Recognition of viral PAMPs

Answer 13

1. Virus enters the cells
2. TLR or other pattern recognition receptor recognizes the viral genome in endosomes and cytoplasm of the cells
3. Pro-inflammatory cytokines and type-1 interferons are produced
4. Interferons alpha and beta establish an anti-viral state in all cells within the vicinity (interferons interfere with viral replication)
5. Immune cells are recruited to site of infection

Question 14

Purpose of Type 1 interferons

Answer 14

• Includes interferons alpha and beta
• They create an environment in which the virus cannot replicate preventing spread into blood and other organs

Ex. raising body temperature to make it more difficult to replicate
Ex. increase expression of ligands on infected cells for NK cell receptors
Ex. increase activation NK cells to kill virus-infected cells

Question 15

Respiratory viral infection example

Answer 15

• Virus enters the alveoli cells of the lungs
• Macrophages phagocytose virus, and travel to lymph node an act as antigen presenting cells to activate T cells which move back to alveoli for

Question 16

Effector cells in Th1 response

Answer 16

• CD4+ T effectors
• CD8+ T effectors
• B cells

Question 17

CD4+ T cells during Th1 response

Answer 17

• Secrete interferon gamma to activate macrophages
• Secrete interferon gamma to drive the Th1 response and enhance CD8+ T cell killing

Question 18

CD8+ T cells during Th1 response

Answer 18

• Recognize infected cells via MHC I and peptide
• Kill via perforin/granzyme and Fas-FasL pathways

Question 19

B cells during Th1 response

Answer 19

• IgG antibodies- used to neutralize virus that is leaving a cell and to opsonize viral antigen on the membrane of infected cells
• Not as much of an antibody response compared to Th2

Question 20

Main mechanisms of Th1 response to overcome viral infection

Answer 20

1. CD8 cytotoxicity
2. Macrophage activation
3. Antibody dependent cell-mediated cytotoxicity (NK cells have Fc-receptors which bind to specific antibodies found on the infected cells. Interaction causes release of granules to kill infected cells)

Question 21

Immune regulation by viruses

Answer 21

There are many ways in which viruses have evolved to avoid the immune response

Question 22

Example of viral immune suppression (viral evolution to avoid immune response)

Answer 22

• HIV
• Virus integrates into the genome of CD4+ T cells, and eventually re-emerges and depletes the T cell population leading to AIDS

Question 23

Example of a cytokine storm (viral evolution to avoid immune response)

Answer 23

• COVID 19 or 1918 pandemic influenza
• Hyperactivation of inflammatory cytokine response; completely out of control

Question 24

Bacteria

Answer 24

• Gram negative, gram positive, acid fast
• Cocci, bacilli, spiral shaped
• Have conserved motifs (LPS, peptidoglycan, CpG DNA, etc.) that can be recognized by TLRs

Question 25

Bacteria mode of transmission

Answer 25

• Infections at many different sites
• Transmission includes contamination of food, instruments, fomites, direct contact, aerosols, etc.

Question 26

Virulence mechanisms of bacteria

Answer 26

• There are different immune responses to different bacterial species

Includes:
- Endotoxins (inside) and exotoxins (secreted)
- Spores and biofilms (persistence in environment, on surgical tools)
- Granulomas (virus remains latent and evades immune system)
- Intracellular cell-cell replication (syncytia)

Question 27

Bacteria intracellular vs extracellular

Answer 27

• Extracellular: Th2 response
• Intracellular: Th1 response

Question 28

Virulence factors

Answer 28

Secretion systems export toxins and directly inject them into host cells

Question 29

Innate response to bacteria

Answer 29

1. Breach of primary barrier
2. Recognition of PAMPs by TLR. Triggers macrophages to release cytokines, chemokines, and anti-microbial peptides
3. Results in vasodilation and increased vascular permeability permits neutrophil and macrophage/DC migration
4. Combination of phagocyte recruitment to the site of infection, cytokines, and anti-microbial peptides. Causes swelling, pain, heat, and redness

Question 30

Alternative activation of complement (bacteria)

Answer 30

1. Motifs of bacteria activate the complement through alternative pathway
2. C3b can opsonize bacteria which promotes the phagocytosis by macrophages, neutrophils, dendritic cells
3. C3a and C5a are anaphylatoxins, promoting inflammation and phagocyte recruitment
4. Membrane attack complex (MAC) punches holes in bacterial cell walls

Question 31

Th2 immunity to extracellular bacteria

Answer 31

• Antigen presenting cells present bacterial peptide to CD4+ Th cells. Results in CD4+ T cells producing Th2 cytokines, and results in the release of IL-4, IL-5, IL-13, and the activation of B cells to produce antibodies
• B cells become plasma cells that produce the antibodies that are pumped into the blood

Question 32

Antibodies job during Th2 immunity response

Answer 32

1. Neutralize toxins (endotoxins, and exotoxins)
2. Opsonization (promote phagocytosis)
3. Neutralize bacterial attachment to cells
4. Activate complement (classical activation)

Question 33

Th1 immunity to intracellular bacteria

Answer 33

1. Intracellular bacteria enters host cells, begins to replicate
2. TLRs inside the cells will detect bacteria and drive a Th1 reponse
3. Cell mediated immunity and the production of interferon gamma (activates macrophages and clears bacterial infection)

Question 34

Parasites

Answer 34

Well developed invaders. Developed to evade the immune responses of the host and to cause minimal reactions so that they can persist and use host resources for a long time

Question 35

Immune responses to parasites

Answer 35

1. Protozoa (Th1 or Th2 response)
2. Helminths (Th2 response)
3. Arthropods (Th1 or Th2 response)

Question 36

Extracellular protozoa with intracellular replication

Answer 36

• Ex. Toxoplasma
• Immune response is generally Th1 and involves the activation of macrophages through interferon gamma which clear the infection
• Extracellular activation will result in antibodies (opsonization , agglutination, and complement activation)

Question 37

Extracellular protozoan

Answer 37

• Ex. African trypanosomes
• Present in tissues and blood and transmitted through tsetse flies. Devastates cattle population
• Immune response is typically through antibody production
• Effective immune response avoidance by switching and shuffling gene expression makes it nearly impossible for the antibody response to keep up because the surface structure (glycoproteins) changes so much and antibodies can’t bind
  » Results in waves of different trypanosomes. When immune response applies pressure, parasite changes

Question 38

Helminths

Answer 38

The immune system is not well equipped to control helminth infections since these organisms often are very well adapted and cause little inflammation or disease

Question 39

What makes helminths hard to destroy?

Answer 39

• Too big to be phagocytosed
• Have thick extracellular cuticle that protects worm from attack by the MAC of the complement system

Question 40

Th2 immunity of Helminths

Answer 40

Immune response results in the production of IgE which cause mast cell degranulation that act to expel the worms
- Basically an allergic response to salivary antigens of the helminth causing worms to detach from the intestinal wall and pass out in feces

Question 41

Eosinophils and helminths

Answer 41

• Eosinophils have Fc receptors and will bind to antibody-coated helminths, degranulate and release their granule contents onto the worm cuticle
• Most efficient way to kill larvae in tissues and important in controlling helminth numbers

Question 42

Immune response against Arthropods

Answer 42

• Immune response against arthropods is mainly directed at salivary proteins (carrier molecules- haptens and collagen)
• Local inflammation and secretion of antimicrobial peptides and cytokines can make it difficult for attachment and adherence of the arthropod.
  o Restricted blood flow from inflammation inhibits the arthropod feeding

Question 43

Arthropod immune invasion

Answer 43

Saliva has immune modulators that suppress inflammation and the establishment of an innate response. Helps with attachment to host and transmission of pathogens

Question 44

Potential vaccine strategies for arthropods

Answer 44

1. Target immune modulators in the saliva of arthropods (host more capable to launch an immune response)
2. Target midgut antigens of the arthropods (antibodies from the host enter the blood meal of arthropods, disrupt the function of the arthropod)