1. DOMMR Week of 9/28-10/1
2. Objectives Discuss hypercoaguable states
Focus specifically on the inherited hypercoaguable conditions
Briefly describe the mechanism behind each of the inherited thrombophilias
Review the hypercoaguable workup and when it is appropriately done
3. Venous Thromboembolism Most common presentation is DVT of the lower extremity and PE
A risk factor for thromboembolism is found in 80% of patients
Often more than one factor at play
Divided into hereditary and acquired
4. Table 1. Inherited and Acquired Causes of Venous Thrombosis.Table 1. Inherited and Acquired Causes of Venous Thrombosis.
5. Inherited Thrombophilias In the recent past, a genetic cause for thrombophilia was detected in only 5-15% of patients
Limited to antithrombin gene deficiency, protein C+S deficiency, dysfibrogenemia
1993: Discovered Factor V gene mutation (Factor V Leiden)
1996: Discovered the prothrombin G20210A gene mutation
Inherited thrombophilias are most common in Caucasians, rare in African or Asian
In all comers with DVT, the incidence of inherited thrombophilias is 24-37%
Of Caucasian patients who present with initial symptomatic DVT, 12-20% are heterozygous for factor V Leiden and 6% heterozygous for prothrombin G20210A mutation
6. Inherited Thrombophilias Inherited hypercoaguable states
A genetic tendency for venous thromboembolism
Should be suspected in anyone who:
Presents with an unprovoked venous or arterial thromboembolic disease at <45 yrs
2 or more thrombotic episodes in the absence of a risk factor for thrombosis
History of objectively confirmed idiopathic thrombosis in first-degree relative
Thrombosis in an unusual site
Mesenteric veins, dural sinus
Neonatal thromobosis or stroke
History of recurrent fetal loss
7. Inherited thrombophilias Will often present with DVT or PE
More than 50% of cases, thrombosis is provoked by surgery, pregnancy, immobilization, OCP, HRT, or old age
Recurrent venous thrombosis is highest in deficiency of antithrombin, protein C, protein S, greater than one inherited thrombophilia, homozygous for factor V Leiden
Those heterozygous for factor V Leiden and prothrombin gene mutation have not been shown to have a higher rate of recurrent venous thrombosis verses the general population
8. Figure 1. Major Mechanisms Involved in the Normal Control of Coagulation and Inherited Thrombophilias. Control of coagulation is achieved by the protein C pathway and antithrombin. In the protein C pathway thrombin bound to thrombomodulin activates protein C, which in turn inactivates activated factor V and factor VIII in the presence of protein S, thereby down-regulating the generation of thrombin. The neutralization of thrombin is achieved by antithrombin bound to heparin sulfate. In the inherited thrombophilias, a deficiency of antithrombin, protein C, or protein S, aberrant activity of factor V, or increased activity of prothrombin results in decreased neutralization of thrombin or increased generation of thrombin.Figure 1. Major Mechanisms Involved in the Normal Control of Coagulation and Inherited Thrombophilias. Control of coagulation is achieved by the protein C pathway and antithrombin. In the protein C pathway thrombin bound to thrombomodulin activates protein C, which in turn inactivates activated factor V and factor VIII in the presence of protein S, thereby down-regulating the generation of thrombin. The neutralization of thrombin is achieved by antithrombin bound to heparin sulfate. In the inherited thrombophilias, a deficiency of antithrombin, protein C, or protein S, aberrant activity of factor V, or increased activity of prothrombin results in decreased neutralization of thrombin or increased generation of thrombin.
10. Factor V Leiden Factor V is activated to Va, which acts as a cofactor in the conversion of prothrombin to thrombin
Normally, Factor Va is degraded by APC and limits prothrombin conversion to thrombin
Arginine is replaced by Glutamine (Arg506Gln) on the factor V gene, resulting in a protein called factor V Leiden
Factor V Leiden is less susceptible to inactivation by APC and is now considered “resistant to APC”
This results in a prothrombotic state
11. Factor V Leiden Most common - 40-50% of inherited thrombophilias
Found in 5% of the Caucasian population
Found in 10-20% of patients with first episode of idiopathic DVT
Found in 50% of patients with recurrent DVT
90-95% of those with factor V Leiden are heterozygous
Homozygotes have a more severe course
Acquired forms of APC resistance found in pregnancy, use of OCPs, elevated Factor VIII or those with antiphospholipid antibodies
12. Factor V Leiden Anticoagulation therapy
Long term therapy not recommended in heterozygotes
At no higher risk of recurrent thrombosis than those without the mutation
In homozygotes, should use prophylaxis in high risk settings
Heterozygous, pregnant women with no history of thrombosis are at low risk for thrombosis
Anticoagulation is not recommended
Recommendations differ if have a history of thrombosis or if Pt is homozygous
14. Prothrombin G20210A Mutation A Vitamin K-dependant protein synthesized in the liver
Due to substitution of adenine for guanine
Results in 30% higher prothrombin levels
This promotes generation of thrombin and impairs inactivation of Factor Va by APC
Found in 2% of the Caucasian population
Seen in 6-10% of patients presenting with first episode of unprovoked DVT
Like with factor V Leiden, there is no increased risk of recurrent DVT in those with the mutation
15. Enhances activity of Protein CEnhances activity of Protein C
16. Protein C deficiency Vitamin K-dependant protein made by the liver
Many different gene mutations are found on the Protein C gene
Among those with mutations on the Protein C gene, levels of Protein C vary widely
Some heterozygotes actually have normal levels
Homozygotes manifest shortly after birth with neonatal purpura fulminans
Heterozygotes are prone to venous thrombosis, but not at increased risk for arterial thrombosis 20% develop thrombosis by 30yrs, 50% by 50yrs
20% develop thrombosis by 30yrs, 50% by 50yrs
17. Protein C deficiency - � Warfarin induced skin necrosis Seen in heterozygotes when giving large loading doses of warfarin and heparin not given concomitantly
Occurs within days of starting therapy and develops over fatty tissue (thigh, buttocks, breasts) or extremities
Begins as a painful erythematous lesion and leads to necrosis
Occurs because of the shorter half life of Protein C verses the other vitamin K-dependent proteins
As a result, protein C levels decrease rapidly once warfarin therapy has been initiated (reduced to 50% of normal within one day)
This effect is even more pronounce in Protein C deficiency
Protein C is lost before the anticoagulant effects of warfarin are established and thrombosis develops
18. Protein C deficiency �Warfarin induced skin necrosis Treatment: stop warfarin, give heparin, Vitamin K, protein C concentrate
Can restart warfarin once skin lesions resolve, restart in low doses and give with heparin
20. Protein S Deficiency Vitamin K-dependant protein
Circulates as both a free protein (40%) and bound C4b-binding protein (60%), which is part of the classic complement system
Only free Protein S can act as a cofactor to APC for the inhibition of Factors Va and VIIIa
C4b is increased in acute phase reactions, causing free Protein S to be decreased
Like in Protein C deficiency, homozygous patients present soon after birth with neonatal purpura fulminans
Protein S is a Vitamin K dependent protein, so levels will be reduced in patients on warfarin
Therefore, must discontinue warfarin therapy at least 1 week prior to testing for deficiency
Protein S is a Vitamin K dependent protein, so levels will be reduced in patients on warfarin
Therefore, must discontinue warfarin therapy at least 1 week prior to testing for deficiency
21. Protein S Deficiency Decreased levels of Protein S in
Liver disease
Renal disease
Women – especially those on OCPs or pregnant
IBD
Neonates, infants
50% of heterozygotes experience DVT by 35yrs
May have atypical presentation: migraine headache, mesenteric vein thrombosis
23. Antithrombin III Deficiency A vitamin K-independent protein that works inhibit thrombin
Prevalence: 1:2000-1:5000 persons
30% of heterozygotes develop a thrombosis by 30yrs, 65% by age 50yrs
Homozygous deficiency is almost always incompatible with life
60% will have recurrent thrombosis
Risk of thrombosis is particularly high in pregnancy
Heparin prophylaxis recommended throughout pregnancy and coumadin for 6 weeks postpartum
24. Testing for hypercoaguable states Acquired and genetic causes frequently overlap
What tests should be ordered?
When should they be ordered?
Will the duration of anticoagulation be affected?
25. Testing for Hypercoaguable States In some settings, up to 50% of Pts with new thrombosis are found to have an abnormality that predisposes to thrombosis
This would suggest routine screening may be of benefit
Patients with factor V Leiden and prothrombin gene G20210A mutation do not have an elevated risk of recurrent thrombosis when compared to patients with venous thromboembolism without the mutation
Currently there are no recommendations to routinely screen for Factor V Leiden or prothrombin gene mutation (the 2 most common inherited disorders)
On the other hand, testing for Protein C and S deficiency and antithrombin deficiency may be warranted because there is an increased risk of recurrent thrombosis after anticoagulation is discontinued
26. Hypercoaguable workup In the setting of acute clot or therapy:
Coumadin reduces protein C and S levels
Heparin can reduce antithrombin levels
Heparin and coumadin make testing for lupus anticoagulant and APC unreliable
Sepsis is associated with reduction in levels of protein C, protein S, antithrombin
27. Hypercoaguable workup APC resistance screen
Clotting assay, then confirm with a genetic test
Prothrombin G20210A mutation
Genetic test (PCR)
Functional assay for Protein C + S, antithrombin III deficiency
Heterozygous deficiencies are from many different mutations and abnormalities
Measure both free and total Protein S
Affected by acute thrombosis and anticoagulation, so check levels at least 2 weeks after completing therapy
Anticardiolipin and lupus anticoagulant clotting assay
Testing should be done at least 2 weeks after completion of anticoagulation
28. Table 3. Diagnostic Tests for Thrombophilias.Table 3. Diagnostic Tests for Thrombophilias.
29. Figure 2. Approach to the Diagnosis and Treatment of Thrombophilia in Patients with Venous Thrombosis. Panel A shows the clinical evaluation of the likelihood of thrombophilia, initial anticoagulant therapy, and the performance of tests. Panel B shows the criteria for continuing therapy and for prophylaxis.Figure 2. Approach to the Diagnosis and Treatment of Thrombophilia in Patients with Venous Thrombosis. Panel A shows the clinical evaluation of the likelihood of thrombophilia, initial anticoagulant therapy, and the performance of tests. Panel B shows the criteria for continuing therapy and for prophylaxis.
30. Review Thrombosis due to acquired and inherited causes:
**Factor V Leiden
Less susceptible to inhibition of APC
“Resistant to APC”
**Prothrombin gene mutation
Protein C deficiency
Protein S deficiency
Antithrombin III deficiency
31. Figure 1. Major Mechanisms Involved in the Normal Control of Coagulation and Inherited Thrombophilias. Control of coagulation is achieved by the protein C pathway and antithrombin. In the protein C pathway thrombin bound to thrombomodulin activates protein C, which in turn inactivates activated factor V and factor VIII in the presence of protein S, thereby down-regulating the generation of thrombin. The neutralization of thrombin is achieved by antithrombin bound to heparin sulfate. In the inherited thrombophilias, a deficiency of antithrombin, protein C, or protein S, aberrant activity of factor V, or increased activity of prothrombin results in decreased neutralization of thrombin or increased generation of thrombin.Figure 1. Major Mechanisms Involved in the Normal Control of Coagulation and Inherited Thrombophilias. Control of coagulation is achieved by the protein C pathway and antithrombin. In the protein C pathway thrombin bound to thrombomodulin activates protein C, which in turn inactivates activated factor V and factor VIII in the presence of protein S, thereby down-regulating the generation of thrombin. The neutralization of thrombin is achieved by antithrombin bound to heparin sulfate. In the inherited thrombophilias, a deficiency of antithrombin, protein C, or protein S, aberrant activity of factor V, or increased activity of prothrombin results in decreased neutralization of thrombin or increased generation of thrombin.
32. Review Factor V Leiden and antithrombin gene mutation are not associated with recurrent thrombosis
Protein C deficiency associated with warfarin induced skin necrosis
Protein S is both free and bound (to C4b binding protein)
Only free protein C can act as a cofactor for APC
Elevated levels of C4b in sepsis, acute phase reactions
Testing should be done after 2 weeks after therapy is concluded (which is typically 6 months)
Decreased levels of Protein C, Protein S, and Antithrombin with acute clot and with treatment
33. Follow Up of patient Was given 6 months of coumadin
Will get high priority (APC resistance, Factor V Leiden gene mutation, prothrombin gene mutation) and intermediated priority testing (protein C deficiency, protein S deficiency, antithrombin III deficiency) 2 weeks after anticoagulation is stopped
