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Drug, Duration and Dose Michael B Streiff, MD FACP Professor of Medicine and Pathology Medical Director, Johns Hopkins Anticoagulation Service Johns Hopkins Comprehensive Hemophilia Treatment Center Chairman, VTE Guideline Committee for the National Comprehensive Cancer Network

Drug, Duration and Dose · Why we need warfarin-Antiphospholipid syndrome • Prospective RCT in triple positive APS • Riva 20 mg (15 mg CrCl 30-50) v. warfarin (INR 2-3) • Rivaroxaban

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Page 1: Drug, Duration and Dose · Why we need warfarin-Antiphospholipid syndrome • Prospective RCT in triple positive APS • Riva 20 mg (15 mg CrCl 30-50) v. warfarin (INR 2-3) • Rivaroxaban

Drug, Duration and Dose

Michael B Streiff, MD FACP

Professor of Medicine and Pathology

Medical Director, Johns Hopkins Anticoagulation Service

Johns Hopkins Comprehensive Hemophilia Treatment Center

Chairman, VTE Guideline Committee for the National Comprehensive Cancer Network

Page 2: Drug, Duration and Dose · Why we need warfarin-Antiphospholipid syndrome • Prospective RCT in triple positive APS • Riva 20 mg (15 mg CrCl 30-50) v. warfarin (INR 2-3) • Rivaroxaban

Disclosures- Michael B. Streiff, MD

• Research support

– AHRQ

– Boehringer-Ingelheim

– Janssen

– NIH/NHLBI

– PCORI

– Portola

– Roche

• Consulting

– Bayer

– CSL Behring

– Daiichi-Sankyo

– Janssen

– Pfizer

– Portola

• Educational Grants

– Covidien

Page 3: Drug, Duration and Dose · Why we need warfarin-Antiphospholipid syndrome • Prospective RCT in triple positive APS • Riva 20 mg (15 mg CrCl 30-50) v. warfarin (INR 2-3) • Rivaroxaban

Why we need warfarin- Body weight

• Nearly 40% of US adults were obese in 2014 (Ogden CL, et al. NCHS

Data Brief, No. 219. 2015)

• Limited number of patients with extremes of body weight in DOAC RCTs (De Caterina R Clin Card Res 2017)

• Weight > 100 kg associated with 2-fold risk of recurrent VTE in RECOVER pooled analysis (Schulman S Circulation 2014)

• Real world survey of 1353 Afib DOAC pts. noted low weight pts. 4-fold higher risk of major bleed (Park CS Heart Rhythm 2016)

• DOAC peak plasma levels below 5th percentile in 21 percent of patients with weight > 120 kg (Piran S et al RPTH 2018)

• ISTH SSC Guidance document suggests DOACs should not be used in patients > 120 kg or BMI > 40 kg/M2 (Martin K et al. JTH

2016)

Page 4: Drug, Duration and Dose · Why we need warfarin-Antiphospholipid syndrome • Prospective RCT in triple positive APS • Riva 20 mg (15 mg CrCl 30-50) v. warfarin (INR 2-3) • Rivaroxaban

Why we need warfarin- Renal Disease

• All DOACs cleared to some extent by kidneys

• DOAC drug levels increase with decreasing renal function

• Patients with poor renal function excluded from the RCTs of DOACS in VTE

– Only 5-8% of participants had CrCl 30-50 ml/min

• Apixaban has been associated with equivalent bleeding and lower thromboembolism in AF

– Retrospective cohort not an RCT

Fanikos J et al Am J Med 2017; Sionitis K et al Circulation 2018

Page 5: Drug, Duration and Dose · Why we need warfarin-Antiphospholipid syndrome • Prospective RCT in triple positive APS • Riva 20 mg (15 mg CrCl 30-50) v. warfarin (INR 2-3) • Rivaroxaban

Why we need warfarin-Antiphospholipid syndrome

• Prospective RCT in triple positive APS

• Riva 20 mg (15 mg CrCl 30-50) v. warfarin (INR 2-3)

• Rivaroxaban associated excess TE

0

2

4

6

8

10

12

14

16

18

20

0 100200300400500600700800

Thro

mb

oe

mb

olis

m, M

ajo

r B

leed

, or

V

ascu

lar

Dea

th (

%)

Days

Riva (N=59) Warf (N=61)

Pengo V et al Blood 2018

HR 7.4

(95% CI 1.7-33)

P=0.008

Page 6: Drug, Duration and Dose · Why we need warfarin-Antiphospholipid syndrome • Prospective RCT in triple positive APS • Riva 20 mg (15 mg CrCl 30-50) v. warfarin (INR 2-3) • Rivaroxaban

Why we need warfarin

• Liver disease

– Patients with elevated AST/ALT/T Bili or Child-Pugh Class B/C excluded from RCTs

• Bariatric surgery

– DOACs absorbed in stomach and small bowel

• Gastrointestinal Bleeding

• Poor Adherence

• Cost

Martin K et al Am J Med 2017

Page 7: Drug, Duration and Dose · Why we need warfarin-Antiphospholipid syndrome • Prospective RCT in triple positive APS • Riva 20 mg (15 mg CrCl 30-50) v. warfarin (INR 2-3) • Rivaroxaban

Duration: Less is more for most

• Classification of Venous Thromboembolism:

– Unprovoked vs. Provoked

– Provoked: Transient vs. persistent risk factor

• A substantial proportion events provoked (Heit JA et

al Arch Intern Med 2002; White RH et al Ann Intern Med 1998; Albertsen IE et al. Am J Med 2018 )

41

25

1518

05

1015202530354045

Perc

ent

White RH et al Ann Intern Med 1998

N=23,564

Page 8: Drug, Duration and Dose · Why we need warfarin-Antiphospholipid syndrome • Prospective RCT in triple positive APS • Riva 20 mg (15 mg CrCl 30-50) v. warfarin (INR 2-3) • Rivaroxaban

Transient risk factors associated with low risk of recurrence

• Metaanalysis of 15 RCT or observational studies

• Follow up 12- 24 months

• Recurrent VTE

– Provoked 3.3% per pt.-yr

– Unprovoked 7.4% per pt-yr

• Limited duration of therapy appropriate for most patients with provoked VTE

0.7

4.2

7.4

0

1

2

3

4

5

6

7

8

Re

curr

en

t V

TE (

% p

er

pat

.-yr

)

N=5159

Iorio A et al Arch Intern Med 2010

Page 9: Drug, Duration and Dose · Why we need warfarin-Antiphospholipid syndrome • Prospective RCT in triple positive APS • Riva 20 mg (15 mg CrCl 30-50) v. warfarin (INR 2-3) • Rivaroxaban

Not all idiopathic VTE recur

0

10

20

30

40

50

60

0 1 2 3 4 5 6 7 8 9 10

Re

curr

en

t V

TE (

%)

Follow Up (years)

Ridker, 2003

Prandoni, 2007

Eichinger,2010

Ridker P et al. NEJM 2003; Prandoni P et al. Haematologica 2007; Eichinger S et al. Circulation 2010

Page 10: Drug, Duration and Dose · Why we need warfarin-Antiphospholipid syndrome • Prospective RCT in triple positive APS • Riva 20 mg (15 mg CrCl 30-50) v. warfarin (INR 2-3) • Rivaroxaban

Bleeding is more deadly then VTE

10

7.4

4.2

0.7

2 2 2 2

0

2

4

6

8

10

12

RecurrentUnprovoked VTE

Unprovoked VTE MedicallyProvoked VTE

SurgicallyProvoked VTE

Perc

ent

Recurrent VTE Major Bleeding

Case Fatality Rate of Bleeding 3 fold higher than VTE!

Rodger M Hematology 2018; Iorio A et al. Arch Intern Med 2010;

Wu C et al. Thromb Res 2014; Carrier M et al Ann Intern Med 2010

Page 11: Drug, Duration and Dose · Why we need warfarin-Antiphospholipid syndrome • Prospective RCT in triple positive APS • Riva 20 mg (15 mg CrCl 30-50) v. warfarin (INR 2-3) • Rivaroxaban

Real World Outcomes Worse than RCT Outcomes

• Retrospective cohort from US 2014-2016

• New diagnosis of VTE starting riva or apix

• In comparison to clinical trial populations, significantly higher events rates

• Real World Outcome rates > RCT rates

0

1

2

3

4

5

6

7

8

Even

ts (

pe

r 1

00

pt-

yr)

Real World Trial

Dawwas GK et al Lancet Hematology 2019; Wu C et al Thromb Res 2014

Rivaroxaban Apixaban

Page 12: Drug, Duration and Dose · Why we need warfarin-Antiphospholipid syndrome • Prospective RCT in triple positive APS • Riva 20 mg (15 mg CrCl 30-50) v. warfarin (INR 2-3) • Rivaroxaban

VTE Duration of Therapy

• Recurrent unprovoked VTE, Antiphospholipid syndrome and other strong thrombophilia-long term therapy

• Cancer-associated VTE- duration of the cancer and its treatment

• First Unprovoked VTE- Assess risk of bleeding and recurrent VTE

• Provoked VTE- limited duration therapy

Page 13: Drug, Duration and Dose · Why we need warfarin-Antiphospholipid syndrome • Prospective RCT in triple positive APS • Riva 20 mg (15 mg CrCl 30-50) v. warfarin (INR 2-3) • Rivaroxaban

HERDOO2 Prediction Rule

• Derived in multicenter cohort of 665 unprovoked VTE pts.

• Low risk women = 1.6% per year vs. High risk women = 14.1% per year

• Recurrent VTE risk in men varied from 3.4% to 19.9% per year

• H = Hyperpigmentation (1 pt.)

• E= Edema (1 pt.)

• R=Redness (1 pt.)

• D= D dimer ≥ 250 mcg/L (1 pt.)

• O = Obesity (BMI ≥ 30) (1 pt.)

• O = Older age (≥ 65 yrs.) (1 pt.)

Low Risk 0-1 pt. High risk ≥ 2 pts.

Rodger M et al Can Med Assoc Journal 2008; Rodger M et al BMJ 2017

Page 14: Drug, Duration and Dose · Why we need warfarin-Antiphospholipid syndrome • Prospective RCT in triple positive APS • Riva 20 mg (15 mg CrCl 30-50) v. warfarin (INR 2-3) • Rivaroxaban

The DASH VTE prediction model

• Based upon meta-analysis of 1818 pts. from 7 studies

• DASH = abnormal Ddimer (2 pts.), Age ≤50 (1 pt.), male Sex (1 pt.) and Hormonal therapy (-2 pts.)

• The DASH score can be used to assess VTE recurrence risk

0

5

10

15

20

25

30

35

40

Lessthan

0

0 1 2 3 4C

um

ula

tive

rec

urr

ent

VTE

at

2 y

ears

(%

)

DASH point score

Derivation Validation

C-statistics: 0.54 for subjects aged > 65 years

versus 0.72 for subjects aged ≤ 65 years).

Tosetto A et al. JTH 2017

Page 15: Drug, Duration and Dose · Why we need warfarin-Antiphospholipid syndrome • Prospective RCT in triple positive APS • Riva 20 mg (15 mg CrCl 30-50) v. warfarin (INR 2-3) • Rivaroxaban

The Vienna Prediction Model

• Prospective cohort of 929 pts. with unprovoked VTE

• F/U 43 months

• Multivariate predictors: Sex, DVT v. PE, D dimer, Peak TG

• The Vienna Model can help estimate recurrence risk

Eichinger S, et al. Circulation. 2010

Version 2: https://cemsiis.meduniwien.ac.at/en/kb/science-

research/software/clinical-software/recurrent-vte/#calc-

params

Page 16: Drug, Duration and Dose · Why we need warfarin-Antiphospholipid syndrome • Prospective RCT in triple positive APS • Riva 20 mg (15 mg CrCl 30-50) v. warfarin (INR 2-3) • Rivaroxaban

Risk Stratification for Recurrent VTE: The Vienna Prediction Model

Eichinger S, et al. Circulation. 2010

Page 17: Drug, Duration and Dose · Why we need warfarin-Antiphospholipid syndrome • Prospective RCT in triple positive APS • Riva 20 mg (15 mg CrCl 30-50) v. warfarin (INR 2-3) • Rivaroxaban

Bleeding Risk Assessment: VTE-BLEED assessment model

• Bleeding RAM derived from RECOVER studies

• Predicts bleeding in AC pts. beyond 1 month

• Low risk (< 2 pts.) 2.8% v. high risk 12.6%

• Validated in Hokusai VTE and XALIA

• May be useful to identify pts. at risk for bleeding

Predictor Points

Active cancer 2

Anemia (Hgb < 12) 1.5

Hx/o Bleeding 1.5

CrCl 30-60 ml/min 1.5

Age ≥ 60 1.5

Male with HTN 1

Klok FA Eur Respir J 2016; Klok FA Thromb Haemost 2017; Kolk FA Brit J Haematol 2018

Page 18: Drug, Duration and Dose · Why we need warfarin-Antiphospholipid syndrome • Prospective RCT in triple positive APS • Riva 20 mg (15 mg CrCl 30-50) v. warfarin (INR 2-3) • Rivaroxaban

DOSE: Is low dose better than standard dose?

• RCT of low (INR 1.5-2) versus standard intensity (INR 2-3) for unprovoked VTE

• Duration of therapy- 2.4 years

• Low dose associated with higher recurrent VTE and similar bleeding

1.9

1.1

4.9

1.9

0.7 0.9

3.7

0.9

0

1

2

3

4

5

6

Even

ts p

er 1

00

pt.

-yea

rs

INR 1.5-2 INR 2-3

P=0.03

Kearon C et al NEJM 2003

Page 19: Drug, Duration and Dose · Why we need warfarin-Antiphospholipid syndrome • Prospective RCT in triple positive APS • Riva 20 mg (15 mg CrCl 30-50) v. warfarin (INR 2-3) • Rivaroxaban

Low dose and standard dose rivaroxaban have similar outcomes• DB-RCT of riva (10 mg

or 20 mg) vs. aspirin for extended treatment after 6-12 mos. of AC

• Median Follow up 351 days

• Low and standard dose rivaroxaban have similar outcomes

1.5

0.5

1.2

0.4

0

0.2

0.4

0.6

0.8

1

1.2

1.4

1.6

Recurrent VTE Major Bleed

Ou

tco

mes

(%

)

Riva 20 mg (N=1107) Riva 10 mg (N=1127)

HR 1.23(0.37–4.03)

Weitz JI et al. N Engl J Med 2017

HR 1.34(0.65–2.75)

Page 20: Drug, Duration and Dose · Why we need warfarin-Antiphospholipid syndrome • Prospective RCT in triple positive APS • Riva 20 mg (15 mg CrCl 30-50) v. warfarin (INR 2-3) • Rivaroxaban

No difference in outcomes with low-dose apixaban

• DB-RCT of apixaban vs. placebo for extended treatment of VTE

• Duration 1 year

• No difference in bleeding or recurrent VTE with low dose versus standard dose apixaban

4.2 4.3

3.8

3.2

0

0.5

1

1.5

2

2.5

3

3.5

4

4.5

5

Recurrent VTE Major or CRNMBleed

Even

ts (

%)

Apixaban 5 mg (N=813)

Apixaban 2.5 mg (N=840)

Agnelli G et al NEJM 2012

RR 0.74

(0.46-1.22)

Page 21: Drug, Duration and Dose · Why we need warfarin-Antiphospholipid syndrome • Prospective RCT in triple positive APS • Riva 20 mg (15 mg CrCl 30-50) v. warfarin (INR 2-3) • Rivaroxaban

Conclusions

• Drug:

– Don’t give up on warfarin

• Duration:

– Most patients do not benefit from indefinite anticoagulation

– Select patients for discontinuation with RAM

• Dose:

– No evidence that low dose safer than standard dose

Page 22: Drug, Duration and Dose · Why we need warfarin-Antiphospholipid syndrome • Prospective RCT in triple positive APS • Riva 20 mg (15 mg CrCl 30-50) v. warfarin (INR 2-3) • Rivaroxaban

Questions ?