1. role of laboratory testing for venous thromboembolism risk factors in guiding therapy Charles Eby M.D
2. Risk Factors for Venous Thromboembolism
3. venous thromboembolism: acquired risk factors temporary
Major trauma
Hip/knee replacement
major surgery
immobilized leg
Acute medical illness
Central venous catheter
Pregnancy/OCP/HRT
“prolonged” travel
persistent
Cancer
Phospholipid antibodies/Lupus Anticoagulant
Previous VTE
4. Incidence of VTE
9. the original thrombophilia trio
Antithrombin protein C protein S
Inheritance: autosomal dominant, incomplete penetrance
Prevalence: 1:2000-5000 1: 200-300 1: 800*
VTE
Prevalence: 1-3% 1-3% 1-3%
relative risk 60-150 6-9 24
* Br J Haem 113: 636-41, 2001
10. Blockbusters of the 1990’s Act. Protein C resistance
>90% factor V Leiden +
Arg506gln eliminates aPC cleavage site in factor Va
5% carriers, U.S. whites
2.3% carriers Hispanics
1.5% carriers U.S. blacks
20% spont.VTE are FVL +
Relative risk:
FVL heterozygous: 7
FVL homozygous: 80 Prothrombin G20210A
30% higher FII activity
2% carriers, U.S. whites
6% spont. VTE are PG 20210 +
Relative risk:
PG heterozygous: 2.8
PG homozygous: ?
11. VTE congenital risk factors: 2003 coagulation regulation:
partial deficiencies: antithrombin, protein C, protein S
coagulation factors:
factor V Leiden , G20210A prothrombin mutation
factors XI, IX, and VIII, fibrinogen
miscellaneous:
dysfibrinogenemia, plasminogen deficiency,diminished fibrinolysis, hyperhomocysteinemia, TAFI, etc.
13. Why order a thrombophilia risk factor laboratory evaluation? To provide an explanation for VTE
To identify risk factors that can be modified
To predict risk of VTE in asymptomatic kin
To assess risk for recurrent VTE
To identify risk factors for pregnancy complications
14. Recurrence rate is minimal for transient VTE risk factors
15. Who is likely to be at increased risk for recurrent VTE? Patients with:
Weak temporary risk factors
Spontaneous DVT/ PE
Onset < 50 years old
Recurrent events
Definitive positive family history in 10 relatives
16. What tests should be included in a thrombophilia evaluation? Antithrombin activity
Protein C activity (clot or chromogenic)
Protein S free antigen
Factor V Leiden first aPC screen, if +, genotype to confirm
Prothrombin G20210A genotype
Homocysteine fasting
Phospholipid antibody IgG+IgM anticardiolipin
Lupus Anticoagulant
17. Thrombophilia testing: �What can go wrong? Misinterpreting temporary decreases in protein C, protein S, and antithrombin as inherited deficiencies
Acute thrombosis
Heparin therapy
Warfarin therapy
Protein S and concurrent pregnancy/OCP use
Poor test precision
Elevated homocysteine due to:
Non-fasting
Ex-vivo release from red cells
18. protein C and antithrombin activities during acute DVT
19. protein S function during acute DVT
20. 2001 College of American Pathology:� coagulation test proficiency Specimen: 70% NPP, 30% buffer
Test range median CV%
Antithrombin 46-121 66 15%
Protein S total 26-61 54 16%
Protein S free 32-70 49 20%
Protein S act 20-86 45 21%
Protein C antigen 30-78 56 19%
Protein C act 34-100 58 16%
21. Thrombophilia testing: what can go wrong? continued Activated protein C resistance (aPCr)
Rarely false positive if pt. plasma is prediluted with factor V depleted plasma
FVL molecular tests
Remote chance of aPCr mutation at alt. site
Prothrombin G20210A
genetic testing is specific and sensitive
22. Thrombophilia testing: what else can go wrong? Phospholipid antibody testing
Phospholipid antibody syndrome diagnosis based on one test result. Confirm persistence
Minimally cardiolipin antibodies, isolated IgA
Commercial labs with long phospholipid antibody panels
No gold standard method for L.A. > 2 screening tests should be performed, and + screen confirmed
23. Do positive thrombophilia tests predict increased risk of recurrent VTE? Based on recent prospective studies
Factor V Leiden (+/-) NO
Prothrombin 20210 (+/-) NO
Anticardiolipin IgG YES
Lupus anticoagulant YES
AT, PC,PS, multiple risks excluded/too rare
24. Candidates for prolonged �(12 months), to indefinite OAT
One VTE and
Phospholipid antibody syndrome
Antithrombin deficiency
Factor V Leiden homozygote?
Combined inherited risk factors (FVL and PG 20210)?
Protein C and S deficiencies?????
6th AACP consensus conference Chest 2001 119(suppl 1)
25. Do global tests of hemostasis predict recurrent VTE? Fibrinolysis
Euglobulin lysis time pre/post venous occlusion
Thrombin generation
Prothrombin fragment F1+2
Thrombin and fibrinolysis
D-dimer levels
26. Risk of VTE recurrence based on D-dimer cut-off of 250 ng/ml
29. Testing asymptomatic kin for thrombophilia risk factors- three cases 33 white male, objectively confirmed spontaneous DVT
30 year old brother with spontaneous DVT one month earlier
Their 58 year old father had spontaneous PE at 28, recurrence after stopping warfarin, on chronic OAT
30. Thrombophilia testing: repeatedly low antithrombin activities (50-60%)
both sons have two children, < 10 years old
Should the 3 daughters and one son be screened for AT deficiency?
If deficient, what kind of prophylaxis should be recommended?
31. VTEs in asymptomatic carriers of AT, Protein C and S deficiencies
33. Case 2 52 white male
First spontaneous DVT 2000, OAT x 6 months
Superficial phlebitis 2002
Second spontaneous DVT 2003
Factor V Leiden heterozygous
2 sons (20’s) and one daughter (18)
Should his children be screened for FVL?
34. VTE risk in thrombophilic FVL+ kindreds
35. Case 3 A 55 year old woman is diagnosed with a DVT 2 weeks after removal of a cast for treatment of an ankle fracture.
Thrombophilia testing is performed, and she is FVL heterozygous. Family history otherwise negative for VTEs.
Should her 25 year old daughter who is taking OCPs be screened?
36. VTE risk in unselected FVL kindreds
37. Prospective study of VTE risk in FVL carriers
38. conclusions Testing for thrombophilic risk factors, both inherited and acquired is recommended for selected patients at high risk for recurrent VTE
Borderline low test results for antithrombin, protein C, and protein S should be viewed with great skepticism due to analytical impression and biologic variability
D-dimer testing may be a useful “global test” to identify patients at lower risk for recurrent VTE
Screening asymptomatic first degree relatives should be tempered by the identified risk factor in the affected proband, and by the “thrombophilic” severity of the kindred.
