Innate Immune System

Question 1

Define infectivity

Answer 1

Infectivity - ability of microbe to establish itself in the host

Question 2

Define virulence

Answer 2

Virulence - capacity of the microbe to cause tissue damage

Question 3

Define the immune system

Answer 3

Immune system =
Cells and organs (eg spleen) that contribute to immune
defences against infectious and non-infectious
conditions (self vs non-self) Cells
Immune system can also recognise non infections conditions eg modified self cells
Immune system can recognise/differentiate self/non self

Question 4

Define infectious disease

Answer 4

Infectious disease =
When the pathogen succeeds in evading and/or
overwhelming the host’s immune defences

Question 5

What are the roles of the immune system

Answer 5

Pathogen recognition = Cell surface and soluble receptors
Foreign microbes cant get anywhere

Containing/eliminating the infection = Killing and clearance mechanisms
Need to be contained so it does not become systemic infection
Want infection to be continues otherwise sepsis
Immune system can contain and deal with infection

Regulating itself = Minimum damage to host (resolution)
Deactivated when threat stopped

Remembering pathogens = Preventing the disease from recurring
Immunisation - remember the microbe
Modified microbe - start immune response, - memory when real microbe encountered - already have the antibodies

Question 6

What is innate immunity

Answer 6

Innate - any microbe has to pass innate immunity
Need to find a path of entry ofpathogen
If it gets through innate - faces specific defences
Innate gives immediate protection - fast
Innate has receptors that have receptors that recognise groups of microbes but very efficient lacks memory - therefore no change in intensity

Question 7

What is adaptive immunity

Answer 7

Adaptive
Would not have adapted if innate not activated
Link between innate - adaptive
Need to activate innate to active adaptive
Adaptive - long lasted - antibodies stay in the blood
But slow
Very specific - can distinguish between different classes of microbes - can recognisedifferent categories of microbes within same group - eg 9 different strains of strep pneumoniae - can recognise the same strain on different epitomes - antigen can recognise this
The morey0u are exposed to same microbe - the Bette =r the immune response is BUT IN THE CASE OF FLU - FLU virus changes all the time.0 scone time = different type of virus -

Question 8

What are the physical barriers to pathogen entry

Answer 8

Skin = physical barrier
Outer part of skin has no blood -
Mucous memb - a lot of secretion - immune - gals malt etc - produces best local response - present in mouth, respiratory tract, Gi tract, urinary tract
Inetsact with environment but provide protection

Question 9

What are physiological barie4s to pathogen entry

Answer 9

• Diarrhoea
• Food poisoning
• Vomiting
• Food poisoning
• Hepatitis
• Meningitis
• Coughing
• Pneumonia
• Sneezing
• Sinusitis

Question 10

What are chemical barriers to pathogen entry

Answer 10

Low pH
Microbesv sensitive to low ph
Staph etc cant grow on skin bc of ph
Stomach low.- acidic - kills anything ingested so nothing gets into intestine
Vagina ph maintained by lactobacillus - produce lactic acid - so bacteria and fungi cannot grow

Antimicrobial molecules
Mucus membrane - form of antibody called IgA produced. IGA binds to microbes and prevents them attaching to membranes etc - in tears, saliva, mucous membrane
Lysozymes - breaks bacterial wall - sebum, perspiration urine
Musus - sticky - cleared by cilia
Beta defensins - epithelium
Epithelium has many antimicrobial molecules
Gastricacid + pepsin- acidic environment used to clear molecules

Question 11

Wha5 ar the biological Barrie’s to pathogen entry

Answer 11

• Normal flora
• Non pathogenic microbes
• Strategic locations
• Nasopharynx
• Mouth/Throat
• Skin
• GI tract
• Vagina (lactobacillus spp)
• Absent in internal organs/tissues
• Benefits
• Compete with pathogens for attachment sites and resources.
• Produce antimicrobial chemicals
• Synthesize vitamins (K, B12, other B vitamins).

Question 12

What are examples of normal flora?

Answer 12

• The skin
• Staphylococcus aureus (week 1, case 1)
• Staphylococcus epidermidis
• Streptococcus pyogenes
• Candida albicans
• Clostridium perfringens
• The nasopharynx
• Streptococcus pneumoniae (week 3, case 2)
• Neisseria meningitidis (week 3, lecture case)
• Haemophilus species

Question 13

How can normal flora cause infection?

Answer 13

Normal flora is displaced from its normal location to
sterile location
• Breaching the skin integrity
• Skin loss (burns)
• Surgery
• Injection drug users
• IV lines 

• Fecal-oral route
• Foodborne infection
• Fecal-perineal-urethral route
• Urinary tract infection (women)

• Poor dental hygiene/dental work
 Common cause of harmless bacteraemia
Bacteria in blood
• Dental extraction • Gingivitis • Brushing/Flossing

⇒ Serious infections in high-risk patients • Asplenic (and hyposplenic) patients • Patients with damaged or prosthetic valves • Patients with previous infective endocarditis -> Antibiotic prophylaxis (UK?)

• Normal flora overgrows and becomes pathogenic when
host becomes immuno-compromised
• Diabetes (session 3, case 2)
• AIDS - drop in t helper cell no
• Malignant diseases - cancer could infiltrate lymphoid organ
• Chemotherapy (mucositis)

• When normal flora is depleted by antibiotics
• Intestine -> severe colitis (Clostridium difficile) • Vagina -> thrush (Candida albicans)

Question 14

What are macrophages

Answer 14

 Present in all organs  Ingest and destroy microbes (Phagocytosis)  Present microbial antigens to T cells (adaptive immunity)  Produce cytokines/chemokines

Question 15

What are monocytes

Answer 15

 Present in the blood (5-7%)  Recruited at infection site and differentiate into macrophages

Question 16

What are neutrophils

Answer 16

 Present in the blood (60% of blood leukocytes)  Increased during infection  Recruited by chemokines to the site of infection  Ingest and destroy pyogenic bacteria: Staph. aureus and Strep. pyogenes

Question 17

What are basophils/mast cells

Answer 17

 Early actors of inflammation (vasomodulation)  Important in allergic responses

Question 18

What are eosinophils

Answer 18

Defence against multi-cellular parasites (worms)

Question 19

What are NK cells

Answer 19

 Kill all abnormal host cells (virus infected or

malignant)

Question 20

What are dendritic cells

Answer 20

 Present microbial antigens to T cells (acquired immunity)

Question 21

Name the receptors on phagocytes and the region o;pathogens which they recognise

Answer 21

Microbial structures:
• Pathogen-associated molecular patterns (PAMPs): Carbohydrates, Lipids, Proteins, Nucleic acids

Phagocytes: • Pathogen Recognition Receptors
(PRRs): Toll Like Receptors - inside and outside cell

Question 22

Give examples of pamps and prrs

Answer 22

See slide

Question 23

What is opsonisation

Answer 23

Opsonisation of microbes: Coating proteins called opsonins that bind to the microbial surfaces leading to enhanced attachment of phagocytes and clearance of microbes

Question 24

Give examples of opsonins

Answer 24

Complement proteins
• C3b • C4b

Antibodies • IgG • IgM

Acute phase proteins
• C-reactive protein (CRP)
• Mannose-binding lectin (MBL)

→ Essential in clearing encapsulated bacteria:
• Neisseria meningitidis
• Streptococcus pneumoniae
• Haemophilus influenzae b

Question 25

Describe phagocytosis

Answer 25

Type late

Question 26

What are phagocyte intracellular killing pathways

Answer 26

Phagocyte intracellular killing mechanisms Oxygen-dependent pathway (respiratory burst)
 Toxic O2 products for the pathogens: Hydrogen
peroxide, Hydroxyl radical, Nitric oxide, Singlet oxygen, Hypohalite
Oxygen-independent pathways
 Lysozyme  Lactoferrin or transferrin  Cationic proteins (cathepsin)  Proteolytic and hydrolytic enzymes

Question 27

What is the complement system

Answer 27

• 20 serum proteins
• Most important C1-C9 • 2 activating pathways
• Alternative pathway
Initiated by cell surface microbial constituents
(endotoxins on E. Coli)
• MBL pathway
Initiated when MBL binds to mannose containing residues of proteins found on many microbes (Salmonella spp. Candida albicans)

Microbe invade
Met my opsonins or antibody
Complement - just remembe rmicrobial properties of 3 yellow boxes
C3a and c5a - recruitment of phagocytes complement product following complement activation - phagocyte attraction - chemical attraction - phagocyte chemical gradient
C3b c4b - opsionantion
C5-c9 - punching hole s- membrane attack complex -killing pathogens

Question 28

Name 2 cytokines and their actins

Answer 28

Anti-microbial actions of macrophage-derived TNFα/IL-1/IL-6

• Liver (opsonins)
• MBL (-> complement activation)
• Bone marrow
• Neutrophil mobilization - act locally
• Inflammatory actions
• Vasodilation • Vascular permeability • Adhesion molecules -> attraction of neutrophils
• Hypothalamus
• Increased body temperature

Question 29

What clinical problems can star with reduced phagocytosis

Answer 29

• Decrease spleen function
• Asplenic patients
• Hyposplenic patients
• Decrease neutrophil number (1.8 109/l)
• Cancer chemotherapy
• Certain drugs (phenytoin)
• Leukaemia and lymphoma
• Decrease neutrophil function
• Chronic granulomatous disease (No respiratory burst)
• Chediak-Higashi syndrome (no phagolysosomes formation)