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Prophylaxis of Venous Thromboembolism in the Medical Patient

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Autopsy revealed 3 fatal PE in the control group. One patient in LMWH group ... PE confirmed by perfusion scan, angiography or autopsy. Lechler 1996 (cont) ... – PowerPoint PPT presentation

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Title: Prophylaxis of Venous Thromboembolism in the Medical Patient


1
Prophylaxis of Venous Thromboembolism in the
Medical Patient
  • Low Molecular Weight Heparin vs. Standard Heparin
  • Melissa Zorn M.D.

2
The Case
  • In general medical patients we frequently employ
    VTE prophylaxis in the form of heparin or
    intermittent pneumatic compression hose. The
    orthopedic population utilizes LMWH for its hip
    fracture patients. If LMWH is better for hip
    fx patients why not use it in general medical
    patients?

3
QUESTIONS
  • How does LMWH differ from UFH?
  • Is LMWH superior to standard UFH in the
    prevention of DVT/PE in the general medical
    patient?
  • Does LMWH have a better side effect profile?
  • Is it cost effective?

4
Risk Factors For VTE
  • Age gt 40
  • Immobility
  • H/O VTE
  • Malignancy
  • Major surgery
  • Hypercoagulable state
  • Obesity
  • Femoral line
  • Varicose veins
  • CHF
  • MI
  • CVA
  • LE fractures
  • Nephrotic syndrome
  • Estrogen use
  • Inflammatory bowel dz

5
LMWH Preparations
  • Name Molecular Weight AntiXaIIa
  • Ardeparin 6000 1.9
  • Dalteparin 6000 2.7
  • Enoxaparin 4200 3.8
  • Nadroparin 4500 3.6
  • Reviparin 4000 3.5
  • Tinzaparin 4500 1.9

6
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7
LMWH vs. UFH
  • More predictable anticoagulant response
  • Better bioavailability at low doses
  • Dose-independent clearance mechanism
  • Longer half life
  • No lab monitoring necessary

8
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9
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10
Dahan 1986
  • RCT, double blind
  • 263 elderly medical patients randomized to
    placebo vs. LMWH (enoxaparin 60mg qd)
  • Groups equal at baseline except slightly higher
    rbc count in placebo, and more malignancy in LMWH
    group
  • 10 day trial, all patients screened routinely
    with 125 I fibrinogen scan

11
Dahan 1986 (cont)
  • RESULTS
  • DVT diagnosed in 12 of 131 (9.1) of placebo and
    4 of 132 (3) of LMWH
  • p0.03
  • Immobilized patients had an incidence of DVT of
    19.5 in subgroup analysis
  • Six patients in each group died

12
Dahan 1986 (cont)
  • Autopsy revealed 3 fatal PE in the control group
  • One patient in LMWH group died of MI and also had
    PE on autopsy
  • One diffuse hemorrhage in LMWH group
    (DIC/malignancy) and two in control
  • Injection site hematomas greater in LMWH group

13
Dahan 1986 (cont)Conclusions
  • LMWH was more effective than placebo in reducing
    DVT in general medical elderly patients.
  • LMWH did not increase the risk of hemorrhage
  • Study size was small
  • Use of 125 I fibrinogen scan to dx DVT

14
Harenberg 1990
  • Randomized, double blind study
  • LMWH (? Sandoparin) qd versus UFH 5,000 units tid
  • 166 General medical patients on bedrest x 1 week,
    study duration 10 days
  • Groups equal except previous VTE, smoking, and
    malignancy higher in LMWH group

15
Harenberg 1990 (cont)Results
  • DVT screened with doppler U/S
  • UFH developed DVT in 4.5 of patients
  • LMWH developed DVT in 3.6
  • p not significant
  • Incidence of hematomas lower in the LMWH group

16
Harenberg 1990 (cont)Conclusions
  • LMWH was equivalent to UFH for the prevention of
    DVT in medical patients
  • PE not addressed
  • Small study size
  • Groups not equal with respect to baseline
    characteristics (LMWH more risk)
  • One death in UFH, three in LMWH

17
Harenberg (hes back) 1996
  • Randomized trial of LMWH (fraxiparine) qd versus
    UFH tid
  • 1590 patients, multicenter trial
  • General medical patients bedridden x 10 days with
    increased risk DVT

18
Harenberg 1996 (cont)
  • PE evaluated if clinically indicated with Q scan
    /- V scan or angiography
  • Baseline groups equal
  • All pts screened with LE dopplers (for proximal
    clots only) on day 1 and 9

19
Harenberg 1996 (cont)Results
  • 4 patients in UFH group developed DVT
  • 6 patients in LMWH group developed DVT (p not
    significant)
  • 23 deaths in LMWH
  • 9 deaths in UFH group (p0.02)
  • Increased death in LMWH not 2ndary to VTE

20
Harenberg 1996 (cont)Results
  • Increased death attributed to poorer prognosis,
    longer bed rest and increased clinical risk
  • Adverse events such as hematomas, erythema, and
    thrombocytopenia higher in UFH group

21
Harenberg 1996 (cont)Conclusions
  • LMWH was as effective as UFH for the prevention
    of DVT in bedridden medical patients
  • LMWH does NOT offer any mortality benefit and may
    present increased mortality
  • Less adverse effects with LMWH
  • Lower incidence DVT ? Only looked at proximal
    disease?

22
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23
Bergmann 1996
  • Multicenter randomized double blind
  • Compared enoxaparin 20 mg qd to UFH bid
  • 423 elderly medical patients evaluated for
    endpoints of DVT and PE
  • DVT screened by 125 I fibrinogen scan

24
Bergmann 1996 (cont)
  • Incidence of VTE in LMWH group was 10/207 (4.8)
    and 10/216 (4.6) in UFH
  • p not significant
  • Adverse events small and similar between groups

25
Bergmann 1996 (cont) Conclusions
  • Enoxaparin was as effective as UFH to prevent VTE
    in bedridden elderly patients
  • Small study
  • No placebo group
  • No mortality benefit seen with use of LMWH
  • Low dose of enoxaparin used (20 qd)

26
Lechler 1996
  • Multicenter randomized double blind trial
  • 959 immobilized medical patients with one or more
    risk factors
  • Enoxaparin 40 mg qd versus UFH tid
  • DVT screened with duplex U/S on days 1 and 7
  • PE confirmed by perfusion scan, angiography or
    autopsy

27
Lechler 1996 (cont)
  • Incidence of VTE in LMWH group was 0.2 and in
    UFH group was 1.4
  • p not significant
  • Two episodes of PE in UFH group and none in LMWH
    group
  • Seven deaths in LMWH group and eleven in UFH group

28
Lechler 1996 (cont) Conclusions
  • LMWH was as effective as UFH for DVT prophylaxis
    in medical patients
  • Trend towards less adverse events in LMWH group
  • Problem low incidence of VTE and PE
  • ? Sensitivity of U/S in asymptomatic patients

29
Kleber 1998
  • Randomized, multicenter open study with blinded
    central reading
  • 451 patients evaluated
  • Enoxaparin 40 mg qd versus UFH tid
  • Published in abstract form only

30
Kleber 1998 (cont) Results
  • 20/239 (8.4) of LMWH group experienced VTE while
    22/212 (10.4) of UFH had VTE
  • Subgroup analysis of CHF patients had a more
    dramatic difference (9.7 in LMWH group and 16.1
    in UFH)
  • Adverse events (bleeding, hematoma, etc) higher
    in UFH group

31
Kleber 1998 (cont) Conclusions
  • Enoxaparin was not inferior to UFH in the
    prevention of VTE in medical patients
  • Published in abstract form only

32
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33
Samama 2000
  • Randomized controlled double blind trial
    comparing enoxaparin 40 mg qd, 20 mg qd, and
    placebo
  • Goals were to determine the incidence of VTE in
    this population of medical patients and to
    distinguish efficacy of different doses versus
    placebo

34
Samama 2000 (cont)
  • Duration of treatment six to fourteen days
  • DVT evaluated by venography or ultrasound, PE by
    lung scan, angio, or CT
  • Primary outcomes assessed in 866 patients
  • Patients evaluated between days one to fourteen
    then reevaluated at day 110

35
Samama 2000 (cont) Results
  • Incidence of VTE in 40 mg group was 5.5
  • In 20 mg group was 15
  • In placebo group was 14.9
  • No significant difference in adverse events or
    deaths in 3 groups
  • Benefit in 40 mg group remained present at day
    110 (prophylaxis ceased)

36
Samama 2000 (cont) Conclusions
  • Enoxaparin 40 mg qd significantly reduced the
    incidence of VTE in medical patients compared to
    20 mg qd or placebo
  • Large numbers of drop outs (21 in all)
  • Drop out rate was similar across all 3 groups

37
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38
Conclusions
  • The incidence of VTE in general medical patients
    varies with different prophylaxis but averages
    9-19 when no prophylaxis is used
  • Heparins in any form reduce the incidence of DVT
  • Low molecular weight heparin is as effective as
    UFH for DVT prophylaxis

39
Conclusions
  • LMWH was NOT proven to be superior to UFH in any
    of the studies
  • LMWH was NOT proven to decrease mortality

40
More Questions
  • Are all the LMWH agents equivalent?
  • What is the appropriate dose and interval of LMWH?

41
What about the hip fx protocol?
  • Some data in the ortho literature suggests LMWH
    may be superior to UFH (Lancet 1992 meta
    analysis)
  • Cochrane Database Systematic Review (2000)
    however stated that insufficient evidence was
    present to establish if LMWH was superior to UFH
    in hip fx

42
What about the squeezers?
  • Intermittent pneumatic compression hose (IPC) or
    SCDs are frequently employed in the medical
    patient population
  • NO trials have been done to establish their
    efficacy in general medical patients
  • Data for IPCs exist in the surgical field in the
    reduction of DVT

43
What about the squeezers?
  • Combined trials of IPCs in general surgery
    patients show a relative risk reduction of DVT of
    60 (25 ---gt 10)
  • IPCs have not been proven to prevent PE in
    general surgery patients
  • Limited data exists regarding ortho patients

44
Recommended Regimens at WFUBMC
45
Cost Comparison of VTE prophylaxis regimens at WFU
46
Back to the case
  • The evidence to date supports using standard UFH
    for DVT prophylaxis in medical patients
  • MORE STUDIES are warranted regarding the use of
    LMWH (especially for medical patients with
    multiple risk factors)
  • The squeezers are indicated when the patient
    cannot tolerate heparin

47
  • Thanks to Pam Pride for reviewing my paper
  • Bill Gates for creating microsoft
  • Al Gore for creating the internet

48
Arriving May 2001
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