Thrombosis and risk factors for thrombosis

Question 1

What does Virchow’s triad define as the causes of thrombosis?

Answer 1

1) Changes to blood flow
2) Changes to blood composition
3) Changes to the vascular endothelium

Question 2

What is the normal cause of arterial thrombosis?

Answer 2

Endothelial injury

Question 3

What kind of thrombus forms in arterial thrombosis?

Answer 3

Platelet rich thrombus

Question 4

What are the 9 risk factors for arterial thrombosis?

Answer 4

1) Smoking
2) Hypertension
3) Hypercholesterolaemia
4) Diabetes
5) Family history
6) Obesity
7) Physical inactivity
8) Age
9) Male sex

Question 5

What are the main pathogenic processes about venous thrombosis?

Answer 5

1) Venous stasis - changes to blood flow

2) Hypercoagulable states - changes to blood constituents

Question 6

What kind of thrombus forms in venous thrombosis?

Answer 6

Predominantly made up of fibrin with a lesser role for platelets

Question 7

How does a DVT present? 3

Answer 7

1) Swollen legs
2) Hot legs
3) Painful legs

Question 8

What percentage of DVTs are clinically silent?

Answer 8

80%

Question 9

What percentage of patients with DVT have asymptomatic PE?

Answer 9

50%

Question 10

DVT is found in what percentage of patients with PE?

Answer 10

> 80%

Question 11

What percentage of patients with VTE develop recurrent VTE in 10 years?

Answer 11

30%

Question 12

What percentage of patients with VTE develop post thrombotic syndrome?

Answer 12

28%

Question 13

What is post thrombotic syndrome?

Answer 13

Chronic leg swelling due to damage to veins when the clots form

Question 14

Why is it important that VTE gets treated?

Answer 14

Mortality of promptly diagnosed and adequately treated from PE is 2%

Question 15

Why is hospital VTE so significant?

Answer 15

Hospital admission is an important predisposing factor for VTE - mixture of immobility and the sorts of things that bring people into hospital

Question 16

What are the 2 strategies for treating VTE?

Answer 16

Prophylaxis:
1) Consistent risk assessment 
2) Appropriate prophylaxis
Treatment
1) Prompt diagnosis
2) Guideline led unified care

Question 17

What are the 5 steps in the care pathway for VTE?

Answer 17

1) Patient admitted to hospital
2) Assess VTE risk
3) Assess bleeding risk
4) Balance risks of VTE and bleeding - offer prophylaxis if appropriate
5) Reassess risk of VTE and bleeding within 24 hours of admission and whenever clinical situation changes

Question 18

What are the 16 risk factors for VTE?

Answer 18

1) Active cancer or cancer treatment
2) Personal history of VTE
3) Age over 60
4) Use of hormone replacement therapy
5) Critical care admission
6) Used of oestrogen containing contraceptive therapy
7) Dehydration
8) Varicose veins with phlebitis
9) Known thrombophilias
10) Obesity
11) One or more significant medical comorbidities (heart disease, metabolic, endocrine or resp pathologies, acute infectious diseases and inflammatory conditions)
12) Pregnancy and post natal period
13) Surgery
14) Immobility
15) Major trauma
16) First degree relative with VTE

Question 19

Name the 2 procoagulant substances in the body?

Answer 19

Platelets and clotting factors

Question 20

Names the 4 anticoagulant substances in the body?

Answer 20

1) Protein C
2) Protein S
3) Anti thrombin III
4) Fibrinolytic system

Question 21

Are aspirin and other antiplatelets appropriate prophylaxis for VTE?

Answer 21

No - remember venous thrombus is fibrin and erythrocyte rich with few platelets

Question 22

What are the 3 important pieces of general advice for avoiding VTE in hospital patients?

Answer 22

1) Do not allow patients to become dehydrated unless it is clinically indicated
2) Encourage patients to mobilise ASAP
3) Do not regard aspirin or other anti platelet drugs as adequate prophylaxis for VTE

Question 23

How do compression stockings work as prophylaxis for VTE?

Answer 23

Graduated compression
From ankle to knee with decreasing compression
Popliteal break
From lower to upper thigh with decreasing compression

Question 24

What are the drugs used as VTE prophylaxis?

Answer 24

1) Low dose low molecular weight heparin
2) Fondaparinux (synthetic pentasaccharide)
Newer anticoagulants:
3) Direct inhibitors of factor Xa - rivaroxaban
4) Direct thrombin inhibitors - dabigatran

Question 25

What is the rough mechanism of action of unfractionated heparin, LMW heparin and Fontaparinox?

Answer 25

Unfractionated heparin, LMW heparin and Fontaparinox work through anti thrombin, they bind to anti thrombin and enhance its effects on thrombin (FII) and/or factor 10a.

Question 26

What is Fontaparinox?

Answer 26

Synthetic pentasaccharide - enhances the effect of anti thrombin on factor 10a

Question 27

How do the actions of unfractionated heparin, LMW heparin and Fontaparinox differ?

Answer 27

Unfractionated heparin has equal effect on thrombin and F10a
LMW heparin has more effect on F10a than thombin
Fontaparinox only acts of factor 10a

Question 28

How does the action of direct thrombin inhibitors differ to other anticoagulants?

Answer 28

Directly inhibit thrombin in an antithrombin-independent way - ie unlike the others do not act by enhancing the effect of anti thrombin but bind directly to thrombin

Question 29

Which is the only anticoagulant which has effect on clot bound thrombin?

Answer 29

Direct thrombin inhibitors

Question 30

What is the function of exclusion tests in diagnosing VTE?

Answer 30

Useful in working out which patients with suspected VTE need to be investigated further and which patients do not

Question 31

What 2 exclusion tests are used in diagnosis of VTE?

Answer 31

1) Wells score: validated numerical clinical probability score
2) Sensitive quantitative D-dimer with high negative predictive value
These are used in an agreed algorithm

Question 32

What are D dimers, how does the test work?

Answer 32

D dimers are break down products of fibrin clot, they are cross link products
They are specific to plasma acting on fribin (ie. don’t get D dimer with plasmin acting on fibrinogen), D dimer tells you a clot has formed and plasmin has broken down the fibrin clot
High D dimer suggests a VTE

Question 33

In patients that need further investigation following exclusion test, what investigation is used?

Answer 33

Duplex scanning (US) with compression to detect and thrombus, it is highly sensitive and specific for diagnosing DVT. Look for loss of flow signal, intravascular defects or non collapsing vessels (a vein with a clot in it will not compress with pressure for US probe) in the venous system

Question 34

What 2 investigations can be used when looking for PE, which is used most commonly?

Answer 34

1) CT PA (pulmonary angiogram)
2) VQ scan
CT PA is most commonly used

Question 35

How does a VQ scan work?

Answer 35

Compare the radio-isotope pattern of injected radio-isotope (perfusion) with inhaled radio-isotope (ventilation)
If the patterns don’t match, ie there is a defect in perfusion but not ventilation there is a V/Q mismatch and this is diagnostic of PE

Question 36

Give 2 LMW heparin drug names?

Answer 36

1) Enoxaparin

2) Tinzaparin

Question 37

How is LMW heparin used to treat VTE? 4

Answer 37

1) Dose fixed by body weight
2) Once daily s/c injection
3) Treat for atleast 5 days
4) Overlap with warfarin until INR >2 for 2 consecutive days (must thus overlap for atleast 2 days)

Question 38

Why is INR a useful measurement when switching from LMW heparin therapy to warfarin?

Answer 38

INR is unaffected by LMW heparin and thus all effect is due to warfarin

Question 39

What are the 5 steps in treatment of uncomplicated in-patient with DVT or PE in whom pregnancy is excluded?

Answer 39

1) Suspect DVT/PE
2) Treat with single does of LMW heparin
3) Confirm diagnosis
4) LMWH for 5 days and start warfarin
5) Overlap LMWH treatment and warfarin until INR is >2 on 2 consecutive days

Question 40

Name 3 oral novel anticoagulants, what is the action of each?

Answer 40

1) Rivaroxaban - Direct 10a inhibitors
2) Apixaban - direct 10a inhibitor
3) Dabigatran - direct 2a (thrombin) inhibitor
(all anti thrombin independent)

Question 41

What are the 4 novel parenteral anticoagulants?

Answer 41

1) Fondaparinux
2) LMWH
3) Argatroban
4) Bivalirudin

Question 42

What is the main advantage of new oral anticoagulants?

Answer 42

Have predictable pharmacokinetics - thus require no monitoring

Question 43

What is the mechanism of action of the oral novel anticoagulant endoxaban?

Answer 43

Direct anti-10a activity

Question 44

What are the 4 main advantages of novel oral anticoagulants over warfarin?

Answer 44

1) Dose is uniform for most patients (warfarin dose can vary 40 fold)
2) No need for monitoring - predictable effect
3) All agents have does reduction recommendations for specific populations eg. very elderly, renal impairment for VTE prevention and for AF
4) Rapid onset of action

Question 45

What is the management for first episode of proximal vein DVT or PE?

Answer 45

Treat for 3-6 mnths

For warfarin target INR = 2.5

Question 46

What is the management for recurrent episodes of VTE?

Answer 46

Treat with long term anticoagulation

Question 47

How does management of DVT or PE which has occurred in the absence of a reversible risk factor differ?

Answer 47

Consider long term anticoagulation

Question 48

What is the management for recurrent VTE on therapeutic anticoagulation?

Answer 48

Increase target INR to 3.5 for warfarin

Question 49

What is the definition of thrombophilia?

Answer 49

Familial or acquired disorders of the haemostatic mechanism which are likely to predispose to thrombosis (inherited abnormalities must co-segregate with clinical thrombosis in the pedigree)

Question 50

There are many families where many members have suffered DVT but there is no abnormality identifiable on investigation (about 50%) of cases, based on this what is the alternative definition of thrombophilia?

Answer 50

Patients who develop DVT:

1) Spontaneously
2) Of disproportionate severity
3) Recurrently
4) At an early age

Question 51

Name the 6 heritable thrombophilias?

Answer 51

Deficiencies of natural anticoagulants:
1) Anti thrombin deficiency
2) Protein C deficiency
3) Protein S deficiency
Abnormalities of pro-coagulant factors:
4) Activated protein C resisitance/ factor V leiden
Abnormalities of fibrin:
5) Dysfibrinogenaemia
6) Prothrombin 20210A

Question 52

What is the difference between activated protein C resistance and factor V leiden?

Answer 52

Factor V leiden is the genotype which leads to the phenotype of activated protein C resistance

Question 53

Name the 1 acquired thrombophilia?

Answer 53

Anti phospholipid syndrome

Question 54

Arterial thrombosis is a clinical feature of which thrombophilia?

Answer 54

Anti phospholipid syndrome

Question 55

Coumarin induced skin necrosis is a clinical feature of which thrombophilia?

Answer 55

Protein C deficiency (warfarin induced skin necrosis)

Question 56

Obstetric complications are a clinical feature of which thrombophilia?

Answer 56

Anti phospholipid syndrome

Question 57

What is thought to be the cause of obstetric complications (recurrent miscarriage) in thrombophilia?

Answer 57

Thrombosis in placental circulation

Question 58

What are the 7 clinical features of thrombophilia?

Answer 58

1) DVT
2) PE
3) Superficial thrombophlebitis
4) Thrombosis of cerebral, axillary, portal and mesenteric veins
5) Arterial thrombosis (APS only)
6) Coumarin induced skin necrosis (PC deficiency)
7) Obstetric complications (APS)

Question 59

What is the action of anti thrombin?

Answer 59

Inhibits factor 10a and 2a (thrombin)

Question 60

How does Protein C become activated?

Answer 60

• Protein C exists in inactive form
• Aswell as cleaving fibrinogen thrombin also binds to thrombomodulin (vascular endothelial protein)
• The thombin-thrombomodulin complex activates Protein C

Question 61

What is the role of activated Protein C?

Answer 61

• Has a co factor called Protein S
• Protein C is responsible fro degrading protein 5 and 8 by proteolysis (which are the co factors in the coagulation cascade)

Question 62

How common are protein C, S and anti thrombin deficiencies?

Answer 62

Altogether account for less than 5% of patients presenting with VTE

Question 63

What is the inheritance pattern of natural anticoagulant deficiencies?

Answer 63

Autosomal dominant

Question 64

What is the genetic defect in Factor V leiden and what is the result of this defect?

Answer 64

Point mutation in factor V gene right at the point where it is cleaved by protein C - thus resistant to activated protein C

Question 65

What is the most common familial thrombophilia?

Answer 65

Factor V leiden

Question 66

How common is Factor V leiden?

Answer 66

European gene - 5-8% of the population heterozygous

Not found in Far east and Africa

Question 67

How does Factor V leiden increase clotting risk?

Answer 67

Heterozygotes - 3-5 fold increase for venous thrombosis
Homozygotes = 30-50 fold increase for venous thrombosis
Interacts with other risk factors for VTE

Question 68

What is prothrombin 20210A?

Answer 68

Point mutation in 3’ untranslated region of prothrombin gene - its an enhancer region responsible for turning on prothrombin synthesis
Associated with increased pro thrombin levels

Question 69

How does prothrombin 20210A increase clotting risk?

Answer 69

3 fold increase in venous thrombosis

Question 70

How common is prothrombin 20201A?

Answer 70

occurs in 1-2% of healthy UK population

Rare in Asia and Africa

Question 71

What is the diagnostic criteria for antiphospholipid syndrome?

Answer 71

Antiphospholipid Ab on atleast 2 occasions 8 weeks apart in association with venous thrombosis or arterial thrombosis or recurrent fetal loss (>2)

Question 72

What is the difference between primary and secondary APS?

Answer 72

APL can be associated with other connective tissue disorders eg. SLE
Primary is APL not in association with other connective tissue disorders

Question 73

Why must a patient have to have evidence of antiphospholipid Ab on more than one occasion to have APS?

Answer 73

They can often be an incidental finding, it is thought we all make these Ab from time to time and most get rid of it
Thus only have APS if they cause a problem and can be identified more than once

Question 74

What 2 test are used to identify antiphospholipid Abs?

Answer 74

1) Lupus anticoagulant

2) Anticardiolipin Ab

Question 75

Is a thrombophilia screen indicated in all patients with VTE?

Answer 75

No

Question 76

Which 3 groups of patients with VTE should have a thrombophilia screen?

Answer 76

1) younger patients
2) Positive family history
3) if discovery of a thrombophilia will change management

Question 77

When should a thrombophilia screen be undertaken?

Answer 77

Not in acute VTE - this will affect results
Not when patient still on Anticoagulant
Preferably not when patient is pregnant or taking OCP
Ie. when patient has recovered from VTE and stopped therapy

Question 78

Which is the only type of thrombophilia which should be screened for in patient with arterial events or recurrent miscarriage?

Answer 78

Anti phospholipid Ab screen only