1. Hypercoagulable States
Sheri Ziegler, DO

2. Virchow’s Triad Medication Acquired PICC line Hereditary Port –a-cath
Cancer
PICC line
Port –a-cath
Immobility

3. Forming a clot Platelets Clotting factors
(I, II, V, VII, IX, X, XI, XII, XIII)
Fibrin
Thrombosis

4. Protein C, Protein S, Antithrombin III
Coagulation Pathways
Intrinsic Pathway
Extrinsic Pathway IX
Tissue Factor + VII
Contact
TF Pathway X XI
TF-VIIa PL
Common Pathway
XIIa
HKa
Prothrombin
XIa PL
IXa
VIIIa PL Xa
XIII Va
(Prothrombinase)
Thrombin
Protein C, Protein S, Antithrombin III
XIIIa
Fibrinogen
Fibrin
(weak)
Fibrin
(strong)

5. Case 1
35 yr old F presents with painful left leg x 1 week

6. History
Trauma
Medications
Family History
Personal History
Immobility

7. Deep vein thrombosis
Ultrasound

8. Acutely became short of breath
What’s worse
Lots of pain
Little pain

9. Pulmonary embolism
CT scan
V/Q scan

10. Pulmonary Embolism

11. Cerebral vein thrombosis

12. Arterial Thrombosis

13. Hypercoagulable States Definition
Clinical situation wherein patients suffer from recurrent venous and/or arterial thrombotic problems or are predisposed to such problems

14. Hypercoagulable States Fine Balance in Hemostatic system
"pro" hemostatic system (procoagulant)
"anti" hemostatic system (anticoagulant)
perturbations in either system can predispose to
clotting or bleeding

15. Hypercoagulable States Acquired Hemostatic Abnormalities
Lupus anticoagulant
Nephrotic syndrome
DIC
Prior thrombosis
Immobilization
Malignancy
TTP
Heparin induced thrombocytopenia
Myeloproliferative disorders
Estrogens
Prolonged travel

16. What patients with a thrombosis should you suspect as having a hereditary hypercoagulable state ?

17. Possible Hereditary Defects predisposing to Venous Thrombosis
DVT < age 45
Positive family history
Recur without precipitating factors
Occurs at atypical site
Idiopathic

18. Incidence of Hereditary Coagulation Defects

19. “Hypercoagulable work-up”
Factor V Leiden mutation
Genetic test for prothrombin gene mutation
Functional assay of antithrombin III
Functional assay of protein C
Protein S assay
Tests for antiphopholipid syndrome

20. Activated protein C Resistance
MOST COMMON ETIOLOGY of hereditary venous thrombosis
Variation among different populations
5% European or Caucasian population
Rare in African Americans, native American Indians, Asians
First described in 1994
Factor V Leiden mutation

21. Protein C, Protein S, Antithrombin III
Cascade
Intrinsic Pathway
Extrinsic Pathway IX
TF Pathway
Tissue Factor + VII
Contact X XI
TF-VIIa PL
Common Pathway
XIIa
HKa
Prothrombin
XIa PL
(Tenase)
IXa
VIIIa PL Xa
XIII Va
(Prothrombinase)
Thrombin
Protein C, Protein S, Antithrombin III
XIIIa
Fibrinogen
Fibrin
(weak)
Fibrin
(strong)

23. Factor V Leiden Characteristics
15-20% of patients with venous thromboembolism
Recurrent thrombosis, familial thrombosis, thrombosis assoc. with pregnancy or young patients

24. Factor V Leiden heterozygous
First Episode of DVT
Relative Risk
Incidence/yr (%)
Normal 1
0.008
Oral contraceptives 4
0.03
Factor V Leiden heterozygous 7
0.06
FVL + OCP 35
0.3
Factor V Leiden
homozygous 80

25. Protein C/S and ATIII Deficiency
All much higher risk of thrombosis
Young age multiple VTE
Usually life long anticoagulation

26. Protein C, Protein S, Antithrombin III
Cascade
Intrinsic Pathway
Extrinsic Pathway IX
TF Pathway
Tissue Factor + VII
Contact X XI
TF-VIIa PL
Common Pathway
XIIa
HKa
Prothrombin
XIa PL
(Tenase)
IXa
VIIIa PL Xa
XIII Va
(Prothrombinase)
Thrombin
Protein C, Protein S, Antithrombin III
XIIIa
Fibrinogen
Fibrin
(weak)
Fibrin
(strong)

27. Prothrombin gene mutation
First described in 1996
Mutation G20210A (guanine to adenine)
Increased thrombosis
Increased prothrombin levels
2.8 fold increased risk of thrombosis
0.02%/year risk of thrombosis

28. Protein C, Protein S, Antithrombin III
Cascade
Intrinsic Pathway
Extrinsic Pathway IX
TF Pathway
Tissue Factor + VII
Contact X XI
TF-VIIa PL
Common Pathway
XIIa
HKa
Prothrombin
XIa PL
(Tenase)
IXa
VIIIa PL Xa
XIII Va
(Prothrombinase)
Thrombin
Protein C, Protein S, Antithrombin III
XIIIa
Fibrinogen
Fibrin
(weak)
Fibrin
(strong)

29. CASE 45 yr old F with acute pain in right foot.
Rash located on arms and legs.
History of recurrent fetal loss.

30. Arterial Thrombosis Evaluation
Lupus anticoagulant
Anticardiolipin antibody
Homocysteine levels

31. Antiphospholipid syndrome
A clinical diagnosis characterized by arterial and venous thrombosis and recurrent fetal loss
Persistent lupus anticoagulant or anticardiolipin antibodies
Thrombocytopenia and livedo reticularis

32. Lupus Anticoagulant Tests
Dilute Russell Viper Venom Time (dRVVT)
Elevated PTT
Anticardiolipin antibody

33. CASE 80 yr old F with DVT. No previous hx of DVT/PE
Not feeling well recently.
Lost 15 pounds in 2 months but, increased abdominal girth.

35. Venous thrombosis in cancer
Common (20%) of all patients with cancer
Increased risk of recurrent VTE
Increased risk bleeding with anticoagulation

36. DVT and Cancer
Current evidence does not support extensive search for occult malignancy
Pursue signs/symptoms
Appropriate screening cancer tests

37. Cancer Screening CBC Chemistry panel Stool for occult blood/colonscopy
PSA and digital rectal exam
Mammogram
Pelvic examination
Urinalysis

38. Now you’ve diagnosed – how do you treat?

39. Therapy of DVT/PE Heparin Warfarin Thrombin inhibtors
Unfractionated (IV)
Low molecular weight (SQ)
Fondaparinux (SQ)
Warfarin
Thrombin inhibtors
Oral Factor Xa inhibitors
Rivaroxaban
Apixaban

40. LMWH Mainly Anti-Xa activity with some antithrombin activity
Long duration of action
More consistent therapeutic window
Not reversible with protamine
Included:
Enoxaparin (Lovenox)
Dalteparin (Fragmin)
Tinzaparin (Innohep)
Fondaparinux (Arixtra) – only anti-Xa activity

41. Coumadin

42. Warfarin—Mechanism of Action
Vitamin K II
Vitamin K Utilization Reduced
VII IX X
Warfarin

43. Effect of warfarin on clotting factors

44. Kaplan-Meier Estimates of the Probability of Symptomatic Recurrent Venous Thromboembolism among Patients with Cancer
Lee, A. et al. N Engl J Med 2003;349:

45. Warfarin—Contraindications
Risk of hemorrhage is greater than benefits of therapy
Pregnancy
Hemorrhagic tendencies or blood dyscrasias
Traumatic surgery with large open areas, recent or contemplated surgery of CNS or eye
Bleeding tendencies with active ulceration or overt bleeding
Lack of patient cooperation
Spinal puncture and procedures with potential for uncontrollable bleeding

46. Long time coming….

47. Thrombin inhibitor Dabigatran (Pradaxa)
Thrombin is key step in thrombosis
Turns fibrinogen into clot
Activates platelets
Activates clotting factors

48. DVT treatment
NEJM: 361: , 2009

49. Bleeding

50. Oral Factor Xa inhibitors
Rivaroxaban (Xarelto)
Apixaba (Eliquis)

51. DVT treatment

52. Bleeding

53. Duration of Therapy
First event with reversible or time limited risk factor
3-6 months
Unprovoked VTE
At least 6 months
Special situations – life long
Cancer – until resolved
Antithrombin III, multiple genetic defects, antiphopholipid syndrome

54. Accept risk of recurrent disease
6 Months Coumadin
INR =
Continue

55. Recurrent Venous Thrombosis
Incidence of DVT (%)
Years

56. D-dimer and Recurrent VTE (PREVENT)
Patients with 1 prior VTE Patients with >1 prior VTE

57. Oral Direct Xa Inhibitor
Xarelto (Rivaroxaban)
Oral agent
Do not need to check INR
Can not be reversed

58. The End