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Ravi Sarode, MD
Professor of Pathology
Chief of Pathology and Medical Director of Clinical Laboratory Services
Director, Transfusion Medicine and Hemostasis
UT Southwestern Medical Center, Dallas, TX
Review of Newer Antiplatelets,
Antithrombotics and Reversal
SVIN Hollywood, FL, November 7, 2014
Disclosures
Consultant CSL Behring
Advisor Octapharma
Off label use of drugs – PCC and
rFVIIa
Please don’t show
coagulation
cascade!!!
Sites of action of Oral Anticoagulants
TF + VIIa
FX
FIX
FXa
FIIa
FIXa FVIIIa
FII
Rivaroxaban
Apixaban
Dabigatran
etexilate
Warfarin
Evolution of Oral
Anticoagulation Therapy
Warfarin to Dabigatran to Rivaroxaban to Apixaban to……..
Dabigatran
Etexilate
(Pradaxa)
Rivaroxban
(Xarelto)
Apixaban
(Eliquis)
MOA Direct
Thrombin
inhibitor
Direct FXa
inhibitor
Direct FXa
inhibitor
Manufacturer Boehringer
Ingelheim
Bayer
Bristol Myers
and Sqibb
Indications 1. Reduce risk
of stroke and
TE in NV-AF
2. Treatment and
prophylaxis of
DVT/PE
1. Reduce risk of
stroke and TE in
NV-AF
2. Rx of DVT and
PE
3. DVT
prophylaxis
1. Reduce risk
of stroke and
TE in NV- AF
2. Rx DVT and
PE
3. DVT
prophylaxis
Target Specific Oral Anticoagulants
RE-LY Study
(n=)
110 mg Dabi
(6015)
150 mg Dabi
(6076)
Warfarin
(6022)
P=value
D/C at 1 yr (%) 14.5 15.5 10.2
Primary outcome –
Stroke/TE (%/yr)
1.53 1.11* 1.69 *<0.001
MI (%/yr) 0.72 0.74 0.53* <0.48
Intracranial Bleed 27 (0.23)* 36 (0.30)* 87 (0.74) <0.001
Extracranial bleed 299 (2.51) 342 (2.84) 315 (2.67) NS
GI Bleed 133 (1.12) 182 (1.51)* 120 (1.02) *<0.001
Life-threatening
Bleed
145 (1.220)* 175(1.45)** 212(1.8) *<0.001 and
**<0.04
No information on how these bleeds were managed!
Connolly NEJM 2009
ROCKET-AF
Outcome Rivaraxoban (20 mg OD)
Warfarin P value
Primary outcome
(Stroke/TE) %/yr
1.7 2.2 <0.001
Major bleeding %/yr 3.6 3.4 NS
ICH 0.5 0.7 0.02
GI Bleed 3.2 2.2 0.001
Hb ↓ >2 g 2.8 2.3 0.02
RBC Tx 1.6 1.3 0.04
Critical bleeding 0.8 1.2 0.007
Fatal bleeding 0.2 0.5 0.02
No information on how these bleeds were managed!
Patel NEJM 2011
ARISTOTLE
Outcome Apixaban (5 mg bid)
Warfarin P value
Primary outcome
(Stroke/TE) %/yr
1.27 1.60 <0.01
Major bleeding %/yr 3.6 3.4 NS
ICH 0.33 0.8 <0.001
GI Bleed 0.76 0.86 NS
Major or clinically relevant
non-major bleeding
4.07 6.01 <0.001
Any bleeding 18.1 25.8 <0.001
Net clinical outcomes –
stroke, TE, or major bleed
3.17 4.11 <0.001
Granger NEJM 2011
FDA approved TSOAs – but never
asked
How bleeds with TSOAs were managed?
How to detect drug levels if needed?
What is the therapeutic level?
Is there a reversal agent for urgent
surgery or serious bleeding?
Is patient’s weight important?
Assessment of compliance?
FDA
Warfarin Dabigatran Rivaroxaban Apixaban
Onset of action 2-5 days 0.5-2 hrs 1-4 hrs 3-4 hrs
Dosing Once a day Twice a day Once a day Twice a day
Bioavailability
(%)
90 4-10 60-80 50%
Prodrug No Yes No No
Variability Common Uncommon Uncommon Unknown
Therapeutic
Index
Narrow Not known Not known Not known
Diet/ drugs ++++ + Not known +
Monitoring
needed
Yes No No No
Test to monitor INR ?? ?Anti-Xa
assay
?Anti-Xa
assay
Elimination half
life
20-60 h 12-17 hrs 6-9 hrs 12 hrs
Renal Excretion Liver 85% renal 33% renal 25% urine
Antidote PCC/FFP/Vit K None None None
How to Manage Bleeding?
Hemostasis and Thrombosis
Research Society (HTRS)
Discontinue the drug
Supportive care
Activated charcoal for dabigatran
Dialysis or PLEX
PCC – either 3 or 4 factor non-
activated may be used
Did not recommend rFVIIa or plasma
Kaatz et al, AJH 2012
Removal of Drugs
Dabigatran Rivaroxaban Apixaban
Within 2-3 hrs Activated
charcoal
? ?
Dialysis 65% free – yes 65% Bound – No 87% bound–No
PLEX No Yes Yes
Line placement Problem Problem Problem
PLEX = Plasma exchange
Experimental Reversal of TSOAs
Prothrombin Complex Concentrate (PCC)
3 factor PCCs = Bebulin, Profilnine
4 factor PCC = Kcentra
Activated PCC = FEIBA
rFVIIa
Variable efficacy in controlling bleeding after
rat tail clipping, head trauma, etc
Ex vivo studies in human volunteers
rVIIa less effective than PCCs
Anticoagulants, Clinics in Lab Med Sep 2014
Rationale for PCC Use
Prothrombin gene mutation - increased levels of FII or prolongs t/2 With thrombophilia have levels >125%
Probably generates more thrombin
PCC - 50U/kg will increase FII and X significantly Generate more IIa – neutralize DTI
Generate more Xa – neutralize DXaI
Coagulation factors get activated in-vivo in minutes hence avoid aPCC
Ostermann et al. Thromb Haemost 2007; 98: 790–7
Time
144 96 72 48 24 18 12 6 2 60 30 10 5 Pre
Minutes: Post-Infusion Hours: Post-Infusion
100
200
300
50
100
150
200
200
200
150
100
50
250
150
100
FVII
FI
I FI
X (
%)
FX
Beriplex
15
Mean infusion 200IU/min; Mean dose 3750 IU (150 mL)
PK Healthy Volunteer Study 1001
Factor Levels Over Time
rFVIIa PCC
Scheduled Surgeries
Discontinue 24 hrs before
48 hrs before for procedures with high
risk for bleeding
Longer for patients with compromised
renal function
TT should be normal before surgery for
dabigatran
PT should be normal with no detectable
anti FXa activity for direct FXa inhibitors
Bleeding Management at UTSW
Hospitals
Tests to assess TSOAs effects
TT or PTT if normal – no DTI
anti-Xa assay (LMWH or Rivaroxaban assay)
Hemostatic strategy
STOP the drug
Topical hemostatic agents for epistaxis
PCC (KCentra) = 4000 Units (fixed dose)
Check above tests 30 min later
Assess clinical effect – may repeat PCC
22
TSOAs
vs
VKA
Newer Antiplatelet Drugs
Nature Review Cardiology 2014
Nature Review Cardiology 2014
Oral APAs
MOA = mechanism of action; P2Y12 = ADP receptor;
Features ASA Ticlopidine Clopidogrel Prasugrel Ticagrelor
MOA COX-1 P2Y12 P2Y12 P2Y12 P2Y12
Prodrug No Yes Yes Yes NO
Onset of action Minutes 4-7 days <24 hr <24 hr faster
Steady state of inhibition Hours 8-11 days 3-7 days 3-5 days Hours
Half-line (hr) 0.5 12.5 7-8 7 8-12
Reversible (days) 3-5 7 5 5-9 5
Bleeding risk + ++ ++ +++ ++++
PLT Tx for Urgent surgery No 1 dose 1 dose 1 dose No
PLT Tx for Urgent Eye/Neurosurgery or ICH
One dose Two doses Two dose Two doses Two doses
Elective surgery No wait 7 days 5 days 5 days 5 days
PLT Function Testing for APAs
AA = arachidonic acid; ADP = adenosine diphosphate; ASA = aspirin; Coll = collagen; CT = closure time; EPI = epinephrine; LTA = light transmission aggregometry; N = normal; ND = not done; PFA-100TM = PLT function analyzer; WBA = whole blood aggregation.
Agonists PF-100 TM CT (sec)
WBA/ VerifyNow
LTA Interpretation
EPI >200 ND ↓↓ ASA Effect
ADP N ↓↓↓ ↓ Clopidogrel
↓↓↓ ↓ Ticlopidine
↓↓↓ ↓ Prasugrel
↓↓↓ ↓ Ticagrelor
ADP N N N P2Y12 resistant
AA ND 0/↓ ↓/↓↓ ASA effect
AA ND N N ASA resistant
Vorapaxar (Zontivity)
Selective potent PAR-1 inhibitor that
blocks thrombin-mediated platelet
activation without interfering with
thrombin action on fibrinogen.
Rapidly absorbed with high bio-
availability
VERY long half-life of ~311 h (13 days)
Metabolized by CYP3A4 in the liver.
Significant Bleeding Complications
TRACER trial120 : NSTE-ACS were randomly assigned to
receive either vorapaxar (40mg loading dose and a 2.5 mg
daily maintenance dose) or placebo in addition to APA
therapy.
A significant 35% increase in mod/severe bleeding (7.2%
versus 5.2%; P<0.001) and three fold increase in ICH (1.1%
versus 0.2%; P<0.001) – terminated early.
TRA 2P-TIMI 50 trial - secondary prevention of ischemic
events in patients with known atherothrombotic disease (MI,
ischaemic stroke, PAD)
Ischemic benefit was hampered by a significantly increased
Mod/severe bleeding (4.2% versus 2.5%; P=0.001) and a two
fold increase in ICH (1.0% versus 0.5%; P<0.001) –
terminated early
FDA Approved in May 2014
For clinical use at 2.5mg once daily for the
reduction of thrombotic cardiovascular events in
patients with a history of MI or PAD
It must be used in addition to standard-of-care
antiplatelet therapy because no studies have
investigated vorapaxar monotherapy.
• Higher bleeding risk!
Vorapaxar is contraindicated in patients with a
history of stroke, transient ischemic attack, or ICH
and in those with active pathological bleeding
How to manage severe bleeding?
• rFVIIa
Pharmacologic Agents for Reversing
Effects of Antiplatelet Drugs
rFVIIa
DDAVP
In vitro Thrombin Generation by
rFVIIa
ASA and plavix treated platelets
Studied various does of rFVIIa and standard conc. of AA, ADP and Collagen
Measured Lag Time, peak and total thrombin generation
rFVIIa in 10, 20, 104 and 200 µg/Kg corrected TG in absence of TF
This effect can be important in pts on APA undergoing urgent surgery or bleeding
Recommendation 15-20 µg/Kg
Altman et al, JTH 2006
DDAVP for ASA Treated Patients
VWF release
Elective Cholecystecomy pts
Randomized to get ASA or ASA+DDAVP and control group
Pre-op BT 7.4’ in ASA vs 5.0’ in control
Post-DDAVP BT 5.5’
4/6 in ASA required blood; 5/6 had post-op bleeding episodes
None in DDAVP group
Recommendation: 0.3 µg/Kg IV
Flordal and Sahlin BJS 1993
Take Home Messages
TSOAs related bleeds Stop the drug
50 U/kg PCC
Antiplatelet therapy related bleed Stop the drug
P2Y12 antagonists
2 doses of PLT Jehovah's witness
rFVIIa 20µg/kg
DDAVP 0.3 µg/kg infusion
New Agents are going to kick…….
