Pathology and Immunology

Question 1

What are the type types of autopsy?

Answer 1

• Hospital

- Medico-legal

Question 2

What deaths are referred to the coroner?

Answer 2

Presumed natural - cause of death not known, not seen doctor in last 14 days

Presumed iatrogenic - peri/postoperative, anaesthetic deaths, abortion, complication of therapy

Presumed unnatural - accidents, industrial death, unlawful killing, neglect, custody deaths, war

Question 3

Who makes referrals to coroner?

Answer 3

Doctors  
Registrar of BDM 
Relatives 
Police 
Anatomical pathology technician 
Other properly interested parties

Question 4

Who performs autopsies?

Answer 4

Histopathologists = hospital autopsies, coronial autopsies

Forensic pathologists = coronial autopsy

Question 5

What is the role of the coronial autopsy?

Answer 5

• Who was the deceased?
• When did they die?
• Where did they die?
• How did they die?

Question 6

What does an autopsy consist of?

Answer 6

1. History/Scene
2. External examination
3. Evisceration
4. Internal examination
5. Reconstruction

Question 7

What does an external examination consist of in an autopsy?

Answer 7

Identification ( formal, body modification, gender, jewellery, clothing) - WHO

Disease and treatment - WHY

Injuries - WHY ME

Question 8

What does evisceration consist of?

Answer 8

• Y shaped incision
• Open all body cavities
• Examine all organs in situ
• Remove thoracic and abdominal organs
• Remove brain

Question 9

What does the internal examination consist of?

Answer 9

Heart and great vessels

• Lungs, tracheal, bronchi
• Liver, gallbladder, pancreas
• Spleen thymus and lymph nodes
• Genitourinary tract
• Endocrine organs
• Central nervous system

Question 10

What is a coronial autospy

Answer 10

The coronial autopsy is a systematic scientific examination that helps the coroner determine who the deceased was, when and where they died and how they came about their death.

Question 11

Who instructs the majority of autopsies?

Answer 11

Medico-Legal authority

Question 12

When is inflammation good and when is it bad?

Answer 12

Good - infection and injury

Bad - autoimmunity

Question 13

What are the classifications of inflammation?

Answer 13

ACUTE:

• sudden onset
• short duration
• usually self resolving

CHRONIC:

• slow onset or sequel to acute
• Long duration
• may never resolve

Question 14

Name the cells involved in inflammation?

Answer 14

Neutrophil polymorphs 
Macrophages 
Lymphocytes
Endothelial cells 
Fibroblasts

Question 15

Describe neutrophil polymorphs in inflammation?

Answer 15

Short lived, usually first on the scene and die at the scene, attract other inflammatory cells such as macrophages

Question 16

Describe macrophages in inflammation?

Answer 16

Long lived cells, phagocytic properties, ingest bacteria and debris, may carry debris away, may present antigen to lymphocyte

Question 17

Describe lymphocytes in inflammation?

Answer 17

Long lived (years) produce chemicals which attract in other inflammatory cells, immunological memory

Question 18

Describe endothelial cells in inflammation?

Answer 18

Line blood vessels, make become sticky in areas of inflammation and inflammatory cells adhere to them, become porous to allow inflammatory cells to pass into tissues

Question 19

Describe fibroblasts in inflammation?

Answer 19

Long lived cells, form collagen in areas of chronic inflammation and repair

Question 20

What would a group of macrophages surrounded by lymphocytes be?

Answer 20

A granuloma

Question 21

What is used to treat inflammation?

Answer 21

NSAIDS - inhibit prostaglandin synthase

Question 22

Define: resolution?

Answer 22

Initiating factor removed, tissue undamaged or able to regenerate

Question 23

Define: Repair?

Answer 23

Initiating factor still present, tissue damaged and unable to regenerate - replacement of damaged tissue by fibrous tissue, collagen produced by fibroblasts

e.g.

Heart after MI
brain after CI

Question 24

Name some cells that do regenerate?

Answer 24

hepatocytes 
pneumocytes 
all blood cells 
gut epithelium 
skin epithelium 
osteocytes

Question 25

Name some cells that do not regenerate?

Answer 25

myocardial cells

neurones

Question 26

Define: thrombosis?

Answer 26

A solid mass of blood constituents formed within an intact vascular system during life

Question 27

What are the three things that can predispose for thrombosis?

Answer 27

1. change in vessel wall
2. change in blood flow
3. change in blood constituents

Question 28

What two factors cause blood clots to be rare?

Answer 28

1. Laminar flow - cells travel in the centre of the arterial vessel and dont touch the sides
2. Endothelial cells that line the vessels are not sticky when they are healthy

Question 29

Define: embolus?

Answer 29

a mass of material in the vascular system able to become lodged within a vessel and block it

Question 30

Define: ischaemia?

Answer 30

A reduction on blood flow to a tissue without any other implications

Question 31

Define: infarction?

Answer 31

The reduction in blood flow to a tissue that is so reduced that it cannot support the maintenance of cells in the tissue so that they die (subset of ischaemia)

Question 32

What is end arterial supply?

Answer 32

Organ supplied by only one artery

Question 33

What organs have more than one artery supplying them?

Answer 33

Lungs, liver and parts of the brain

Question 34

What is an embolism?

Answer 34

The process of a solid mass in the blood being carried in the circulation to a place where it gets stuck and blocks the vessel

Question 35

Describe the process

Answer 35

1. Platelet aggregation, as platelets release chemicals when they aggregate which cause other platelets to stick to them starting off the cascade
2. Once the clotting cascade has started there is formation of the large protein molecule fibrin which ,makes a mesh in which red blood cells can become entrapped

Question 36

What are some risk factors of atherosclerosis?

Answer 36

• Cigarette smoking
• Hypertension
• Diabetes
• Hyperlipidaemia

Question 37

How does hypertension increase the risk of atherosclerosis?

Answer 37

Shearing forces damage endothelial cells from hypertension

Question 38

What is apoptosis?

Answer 38

Programmed cell death

BcL12 inhibits caspases
Bax+ stimulates caspases

Question 39

What is HIV? (apoptosis)

Answer 39

Too much apoptosis

Question 40

What is necrosis?

Answer 40

Traumatic cell death

e.g. caseous necrosis - looks like soft cheese - TB

Question 41

Define: Hypertrophy?

Answer 41

It is an increase in the size of a tissue caused by an increase in the size of constituent cells (if they can’t divide then they can only hypertrophy)

Question 42

Define: Hyperplasisa?

Answer 42

It is an increase in the size of the tissue caused by an increase in the number of constituent cells

Question 43

Define: Metaplasia?

Answer 43

A change in the differentiation of a cell from one fully differentiated type to a different fully differentiated type

Question 44

Dysplasia?

Answer 44

An imprecise term for the morphological changes seen in the progression of cells becoming cancer

Question 45

Define:
Congenital
Inherited
Acquired

Answer 45

Congenital = present at birth

Inherited = is caused by a genetic abnormality

Acquired = caused by non environmental factors

Question 46

Name some of the components in the pathology of ageing?

Answer 46

• Dermal elastosis
• Osteoporosis
• Cataracrs
• Senile dementia
• Sarcopenia

Question 47

Define: carcinogenesis?

Answer 47

It is the transformation of normal cells to neoplastic cells through permanent genetic alterations or mutations –> applies to malignant neoplasms

Question 48

Define: oncogenesis?

Answer 48

Benign and malignant tumours

Question 49

What are the differences between:
Carcinogenic
Oncogenic
Mutagenic

Answer 49

Carcinogenic = cancer causing 
Oncogenic = tumour causing 
Mutagenic = acts on DNA

Question 50

What percentage of cancer risk is environmental?

Answer 50

85%

Question 51

What are the problems with working out what is carcinogenic:

Answer 51

• Latent intervals may be decades
• Complexity of environment
• Ethical constraints

Question 52

What is some epidemiological evidence for some carcinogens?

Answer 52

Hepatocellular carcinoma: uncommon in the UK/USA and common in areas with increased hepatitis B/C and mycotoxins

Oesophageal carcinoma: increased incidence in Japan, China Turkey and Iran - dietary factors (hot coffee and Linhsien chickens

Question 53

Name the five classes of carcinogens and give an example for each?

Answer 53

1. Chemical e.g. polycyclic aromatic hydrocarbons
2. Viral e.g. HPV
3. Ionising and non ionising e.g. thyroid cancer in Ukrainian children
4. Hormones, parasites and mycotoxins e.g. oestrogen and breast cancer
5. Miscellaneous e.g. asbestos and metals

Question 54

What are the different types of chemical carcinogen and what tumours do they cause?

Answer 54

1. Polycyclic aromatic hydrocarbons: lung and skin cancer (smoking and mineral oils)
2. Aromatic amines: bladder cancer (rubber/dye workers)
3. Nitrosamines: gut cancer (proven in animals)
4. Alkylating agents: leukaemia (small risk in humans)

Question 55

What are some of the host factors that can increase the risk of cancer?

Answer 55

Race: melanin 
Diet 
Constitutional factors e.g age and gender 
Premalignant lesions 
Transplacental exposure

Question 56

What does leukaemia effect?

Answer 56

Blood

Question 57

What does lymphoma effect?

Answer 57

Lymphocytes

Question 58

What does sarcoma effect?

Answer 58

Connective tissue

Question 59

What does carcinoma effect?

Answer 59

Epithelial tissue

Question 60

Define: neoplasm?

Answer 60

A lesion resulting from the autonomous or relatively autonomous abnormal growth of cells which persists after the initiating stimulus has been removed

Question 61

What is neoplasia? (4)

Answer 61

Autonomous
Abnormal
Persistent
New growth

Question 62

How does neoplasia affect the population?

Answer 62

25% of the population effected at some point in lifetime

Risk increases with age

Accounts for 20% of all deaths

Question 63

Describe the structure of neoplasms?

Answer 63

Neoplasm = neoplastic cells + stroma

Neoplastic cells: derive from nucleated cells, usually monoclonal, growth pattern related to parent cells, synthetic activity related to parent cell e.g. collagen, mucin, keratin hormones etc

Stroma: connective tissue framework, mechanical support, nutrition

Question 64

Describe tumour angiogenesis?

Answer 64

1. Transformed cell
2. Avascular tumour nodule
3. Vascularised tumour
4. Vascularised tumour with central necrosis

Question 65

Why classify neoplasms?

Answer 65

1. To determine appropriate treatment

2. To provide prognostic information

Question 66

What are the methods of classification?

Answer 66

Behavioural: benign/malignant
Histogenetic: cell of origin

Question 67

Describe a benign neoplasm?

Answer 67

Localised
Non-invasive 
Slow growth rates 
Low mitotic activity 
Close resemblance to normal tissue 
Circumscribed or encapsulated

Question 68

Why worry about benign neoplasms?

Answer 68

Pressure on adjacent structures 
Obstructs flow 
Production of hormones 
Transformation into malignant neoplasms 
Anxiety

Question 69

Describe malignant neoplasms?

Answer 69

Invasive

Metastases

Rapid growth rate

Variable resemblance to normal tissues

Poorly defined or irregular borders

Hyperchromatic nuclei, pleomorphic nuclei, increased mitotic activity , necrosis common, ulceration, growth on mucosal surfaces and skin often endophytic

Encroach upon and destroy surrounding tissue, are poorly circumscribed and have crab like cut surface

Question 70

Why worry about malignant neoplasms?

Answer 70

Destruction of adjacent tissue
Metastasies 
Blood loss from ulcers 
Obstruction of plow 
Hormone production 
Paraneoplastic effects 
Anxiety 
Pain

Question 71

Define: histogenesis?

Answer 71

The specific cell origin of a tumour

Question 72

What may neoplasms arise from?

Answer 72

• Epithelial cells
• Connective tissue
• Lymphoid / haemopoetic

Question 73

What is a papilloma?

Answer 73

A benign tumour of the non glandular, non secretory epithelium, prefixed with the cell type of origin e.g. squamous cell papilloma

Question 74

What is an adenoma?

Answer 74

A benign tumour of glandular or secretory epithelium e.g. colonic adenoma

Question 75

What is a carcinoma?

Answer 75

A malignant tumour of epithelial cells, prefixed by the epithelial cell type

Question 76

Give some examples of benign epithelial neoplasms?

Answer 76

Lipoma - adipocytes
Chondroma - cartilage
Osteoma - bone
Angioma - vascular

Question 77

What is a rhabdomyoma?

Answer 77

Benign neoplasm of striated muscle

Question 78

What is a leiomyoma?

Answer 78

Benign neoplasm of smooth muscle

Question 79

Give some examples of some malignant neoplasms? (6)

Answer 79

1. Liposarcoma - adipose tissue
2. Rhabdomyosarcoma - striated muscle
3. Leiomyosarcoma - smooth muscle
4. Chondrosarcoma -cartilage
5. Osteosarcoma - bone
6. Angiosarcoma - blood vessel

Question 80

What is an anaplastic tumour?

Answer 80

Where the cell type is unknown

Question 81

Give some examples of -omas that are NOT neoplasms?

Answer 81

Granuloma
Mycetoma
Tuberculoma

Question 82

What is a melanoma?

Answer 82

Malignant neoplasm of melanocytes

Question 83

What is a mesothelioma?

Answer 83

Malignant tumour of mesothelial cells

Question 84

What is a lymphoma?

Answer 84

Malignant neoplasm of lymphoid cells

Question 85

What is a teratoma?

Answer 85

Embryonal tumours

Question 86

What is a basal cell carcinoma?

Answer 86

It only invades skin locally and never spreads to other parts of the body - complete local excision means total cure

Question 87

What cancers most commonly spread to bone?

Answer 87

1. Breast
2. Prostate
3. Lung
4. Thyroid
5. Kidney

Question 88

Describe a treatment plan for breast cancer?

Answer 88

1. Confirm diagnosis
2. Has it spread to the axilla? - axillary node clearance needed
3. Has it spread to the rest of the body? - chemotherapy

Question 89

What is adjuvant therapy?

Answer 89

Extra treatment given after surgical excision (micrometastasies)

Question 90

Which tumours commonly metastasise to the liver?

Answer 90

• Colon
• Stomach
• Pancreas
• Intestine

Question 91

Describe how cancer metastasises?

Answer 91

1. invasion of the basement membrane
2. Tumour cell motility
3. Intravasation
4. Evasion of the host immune defence
5. Growth at the metastatic site
6. Anigogenesis

Question 92

Define: innate immunity?

Answer 92

Instinctive, nonspecific, doesnt depend of lymphocytes and present from birth

Question 93

Define: adaptive immunity?

Answer 93

Specific accquired/learned immunity requires lymphocytes and antibodies

Question 94

Which cells are the polymorphonuclear leukocytes?

Answer 94

Neutrophil
Eosinophil
Basophil

Question 95

Which cells are the mononuclear leukocytes?

Answer 95

Monocytes - macrophage in tissue
T-cells
B-cells - plasma cell in tissue

Question 96

What are the different types of T-cells?

Answer 96

T-regs
T helper (CD4)
Cytotoxic (CD8)

Question 97

What are the dendritic cells?

Answer 97

Kupffer and Langerhans

Question 98

What is compliment?

Answer 98

A group of 20 serum proteins that need to be activated in order to be functional, activated only as a part of the immune response

They can

1. Lyse microbes directly
2. Chemotaxis
3. Opsonisation (ketchup on chips)

Question 99

Describe igG?

Answer 99

most predominant Ig in human serum - 70-75%

Question 100

Describe IgM?

Answer 100

accounts for for 10% of Ig in serum, pentamer formation requires J chain, mainly found in the blood as its too big to cross endothelium, mainly primary immune response

Question 101

Describe IgA

Answer 101

accounts for 15% of Ig in serum, it is a monomer, predominant Ig in mucous secretion, sIgA held together with a J chain

Question 102

Describe igD?

Answer 102

Accounts for 1% of Ig in serum

Question 103

What are cytokines?

Answer 103

Proteins that are secreted by immune and non immune cells e.g.. inferons and interleukins

Question 104

Function of interferons?

Answer 104

Interferons induce as state of antiviral resistance in uninfected cells and limit the spread of a viral infection

Question 105

Function of interleukins?

Answer 105

Interleukins are produced by many cells and can be pro inflammatory or anti-inflammatory and can cause cells to divide, differentiate and to secrete factors

Question 106

What are colony stimulating factors?

Answer 106

Involved in directed the division and differentiation of bone marrow cells - precursors of leukocytes

Question 107

What are tumour necrosis factors?

Answer 107

TNFα & β Mediate inflammation and cytotoxic reactions

Question 108

What are chemokines?

Answer 108

Chemotaxic cytokines

Group of approx. 40 proteins that direct the movement of leukocytes and other cells from the blood stream into the tissues of lympth organs by binding to specific receptors on the cells

Question 109

Give some examples of chemokines?

Answer 109

CXCL – mainly neutrophils
CCL –monocytes, lymphocytes, eosinophils, basophils
CX3CL – mainly T lymphocytes & NK Cells
XCL – mainly T lymphocytes

Question 110

Give some characteristics of innate immunity?

Answer 110

innate - non specific

• 1st line of defence
• Provides barrier to antigen
• Instinctive
• Present from birth
• Slow response
• No memory

Question 111

Give some characteristcs of adaptive immunity?

Answer 111

adaptive - specific

• response to specific antigen
• learnt behavior
• memory specific to antigen
• quicker response

Question 112

What is innate immunity composed of?

Answer 112

• Physical and chemical barriers e.g. skin, mucous, pH
• Phagocytic cells e.g. neutrophils and macrophages
• Blood proteins e.g. compliment and acute phase

Question 113

Define inflammation?

Answer 113

Inflammation is a series of reactions that brings cells and molecules of the immune system to sites of infection or damage

Question 114

What are the hallmarks of infection?

Answer 114

1. Increased blood supply
2. Increased vascular permeability
3. Increased leukocyte transendothelial migration

Question 115

What is the response to tissue damage?

Answer 115

1. Coagulation - stop bleeding
2. Leukocyte recruitment - acute inflammation
3. Kill pathogens, neutralise toxins, limit pathogen spread
4. Clear pathogens/ dead cells - phagocytosis
5. Proliferatoin of cells to repair damage
6. Remove blood clot - remodel extracellular matrix
7. Re-establish normal structure/function of tissue

Question 116

Describe: acute inflammation?

Answer 116

Complete elimination of a pathogen followed by resolution of damage, disappearance of leukocytes and full regeneration of tissue

Question 117

Describe: chronic inflammation?

Answer 117

persistent unresolved inflammation

Question 118

What senses microbes in:
blood?

tissues?

Answer 118

blood- Monocytes and neutrophils

tissues - Macrophages and dendritic cells

Question 119

What are the different types of compliment?

Answer 119

Classical - Ab bound to microbe
Alternative - C’ binds to microbe
Lectin - activated by mannose binding lectin bound to microbe

Question 120

What are the stages of phagocytosis?

Answer 120

1. binding
2. engulfment
3. phagosome engulfment
4. Phagolysosome
5. membrane disruption

Question 121

What are the mechanisms of microbial killing?

Answer 121

O2 dependent - Reactive Oxygen Intermediate

• Super oxides converted to H2O2 and then .OH free radical
• Nitric oxide = vasodilation, increased extravasation but also antimicrobial

O2 independent

• Enzymes e.g. lysosomes
• Proteins e.g. defensins into membranes
• pH

Question 122

Types of adaptive immunity?

Answer 122

Cell mediated - t cells - intracellular microbes

Humoral Ab - B cells - extracellular microbes

Question 123

What is cell mediated immunity and what does it require?

Answer 123

Interlay between antigen presenting and T cells

Requires intimate cell to cell contact

• To control Ab responses via contact with B cells
• To direct recognise and kill viral infected cells

Question 124

Describe the features of T lymphocytes?

Answer 124

• do not response to soluble antigens only intracellular presented antigens
• T cells that recognise self are kills in the foetal thymus as they mature - T cell selection
• T cell receptor recognises foreign antigens in association with major histocompatibility complex

Question 125

Describe the major histcompatability complex?

Answer 125

• Displays peptides from self or non self proteins e.g. degraded microbial proteins on the cell surface - invasion alert

Question 126

Describe the Major Histocompatability Complex I?

Answer 126

MHC I coded by HLA (A, B & C genes) - glycoproteins on ALL nucleated cells (graft rejection).

Question 127

Describe the Major Histocompatability Complex II ?

Answer 127

MHC II - coded by HLA (DP, DQ& DR) - glycoproteins ONLY on APC (antigen presenting cells

Question 128

Describe the relationship between intrinsic antigens and MHC?

Answer 128

Antigen: Intrinsic antigen (intracellular e.g. virus)

MHC: Class I (all cells)

T cells: Tc (CD8)

Function: kill infected cell with intracellular pathogen

Question 129

Describe the relationship between extrinsic antigens and MHC?

Answer 129

Antigen: extrinsic antigen (extracellular e.g. phagocytosis)

MHC: Class II (apc only)

T cells: Th (CD4)

Function: Help B cells make Ab to extracellular pathogen, can help directly kill

Question 130

Describe secreted and circulating Pattern Recognition Receptors? (PRRs)

Answer 130

Antimicrobial peptides secreted in lining fluids from epithelia and phagocytes e.g. defensins and phagocytes

• Lectins and collectins: carbohydrate containing proteins that bind carbohydrates or lipids in microbe walls, activate compliment and improve phagocytosis e.g. mannose binding lectin, surfactant proteins A and D
• Pentraxins. Proteins like CRP, which have some antimicrobial actions, can react with the C protein of pneumococci, activate complement, and promote phagocytosis.

Question 131

Describe Cell associated Patter Recognition Receptors (PRRs)?

Answer 131

Receptors that are present on the cell membrane or in the cytosol of the cells

• Recognise a broad range of molecular patterns
• TLRs are the main family

Question 132

Describe TLRs?

Answer 132

• Family of receptors that may participate in pathogen recognition and particularly in pathogen phagocytosis
  e. g.
• Mannose receptor on macrophages
• Dectin-1. Widespread on phagocytes, helps recognise beta glucans in fungal walls
• Scavenger receptors on macrophages

Question 133

Describe NLRs?

Answer 133

(type of PRR) Named after the first members of the family, NODs, Nod-like receptors.

Rapidly expanding family of another 22 human proteins that detect intracellular microbial pathogens.

Detection of peptidoglycan, muramyl dipeptide, Best known are NOD1, NOD2, NLRP3 etc

Question 134

Describe NOD2?

Answer 134

(type of PRRs) Widespread expression

Recognises muramyl dipeptide MDP a breakdown product of peptidoglycan

Activates inflammatory signalling pathways

Non-functioning mutations: Crohn’s disease

Hyperfunctioning mutations: Blau syndrome (rare, chronic granulomatous inflammation of skin, eyes and joints)

Question 135

Describe RLRs?

Answer 135

Named after first members of the family: Rig-I. Rig-like helicases = RLRs

Best known are RIG-I and MDA5, who’s roles are to detect intracellular double-stranded viral RNA and DNA.

They couple effectively to activation of interferon production enabling an antiviral response

NOD2 can also activate anti-viral signalling

Question 136

What are some damage molecules?

Answer 136

Extracellular molecules: fibrinogen, hyaluronic acid, tenascin C

Intracellular molecules: for example, HMGB1, mRNA, heat shock proteins, uric acid (and uric acid crystals), stathmin

Question 137

How can TLRs recognise damage?

Answer 137

TLRs also adapted to recognise a range of endogenous damage molecules, which may share characteristics of hydrophobicity.

Appearance of host molecules in unfamiliar contexts can activate TLRs.

TLR signalling by cellular damage products activates immunity to initiate tissue repair and perhaps enhance local antimicrobial signalling.

Question 138

How are PRRs relevent to disease?

Answer 138

Recognition of host molecules in autoimmune disease
Failure to recognise pathogens or increased inflammatory responses

Atherosclerosis, arthritis, COPD, inflammatory bowel disease, etc.

Question 139

How can PRR function translate to therapy?

Answer 139

Enhance TLR signalling: improve immunity, adjuvants

Inhibit TLR signalling: sepsis syndromes, inflammation, arthritis

Modify adaptive immune response: bias Th and Treg responses

Question 140

Describe the differences between immediate and delayed drug hypersensitivity?

Answer 140

Immediate - less than one hour, urticarial, anaphylaxis

Delayed - more than one hour, other rashes, hepatitis, cytopenias

Question 141

What are the four types of hypersensitivity?

Answer 141

Type 1 - IgE mediated drug hypersensitivity
Type 2 - IgE mediated cytotoxicity
Type 3 - Immune complex deposition
Type 4 - T cell mediated

Question 142

Describe type 1 hypersensitivity?

Answer 142

Type 1 - acute anaphylaxis

• Prior exposure to antigen//drug
• IgE antibodies formed after exposure to molecule
• IgE becomes attached to mast cells or leucocytes, expressed as cell surface receptors
• Re-exposure causes mast cell degranulation and release of pharmacologically active substances such as histamine, prostaglandins, leukotrienes, platelet activating factors et c

Question 143

Describe type 2 hypersensitivity?

Answer 143

Type 2 - antibody dependent cytotoxicity

• Drug or metabolite combines with a protein
• Body treats it as a foreign protein and forms antibodies (IgG IgM)
• Antibodies combine with the antigen and complement activation damages the cells e.g. methyl-dopa-induced haemolytic anaemia

Question 144

Describe type 3 hypersensitivity?

Answer 144

Type 3 - immune complex mediated

• Antigen and antibody form large complexes and activate complement
• Small blood vessels are damaged or blocked
• Leukocytes attracted to the site of reaction release pharmacologically active substances leading to an inflammatory process
• Includes glomerulonephritis

Question 145

What are the main features of anaphylaxis?

Answer 145

• Exposure to drug, immediate rapid onset
• Rash (absent in 10%)
• Swelling of the lips, face, oedema, central cyanosis
• Wheeze/SOB
• Hypotension
• Cardiac arrest

Question 146

What drug is intially administered for anaphylaxis?

Answer 146

Adrenaline IM 500 micrograms (300mcg epi-pen)

Question 147

Describe the management of anaphylaxis?

Answer 147

1. Commence basic life support ABC
2. Stop the drug if infusion
3. Adrenaline IM 500 micrograms
4. High flow oxygen
5. IV fluids
6. IV antihistamine
7. IV hydrocortisone

Question 148

Describe effects of adrenaline?

Answer 148

• VASOCONSTRICTION as increase in peripheral vascular resistance, increased BP and coronary perfusion via alpha 1 adrenoreceptors
• Stimulation of Beta-1 adrenoceptors, positive inotropic and chronotrpic effects on the heart
• Reduces oedema and brochodilates via beta-2-adrenoceptors
• Attenuates further release of mediatiors from mast cells by basophils by increasing intracellular c-AMP and so reducing the release of inflammatory mediators

Question 149

What are the medicine risk factors for hypersensitivity?

Answer 149

• Protein or polysaccharide based macromolecules

Question 150

What are the host risk factors for hypersensitivity?

Answer 150

Females > males
EBV, HIV
Previous drug reactions
Uncontrolled asthma

Question 151

What are the genetic risk factors for hypersensitivty?

Answer 151

Certain HLA groups

Acetylator status

Question 152

What is the clinical criteria for an allergy to a drug?

Answer 152

1. Does not correlate with the pharmacological properties of the drug
2. No linear reaction with dose
3. Reaction similar to those produced by other allergens
4. Induction period of primary exposure
5. Dissapearance on cessation
6. Reapperance on re exposure
7. Occurs in a minority of patients on the drug