Everything You Need to Know about Anticoagulation
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Transcript Everything You Need to Know about Anticoagulation
What’s New
in the World of
Anticoagulation
Angela Lambing, MSN, ANP-c, GNP-c
Hemophilia & Thrombosis Treatment Center
Henry Ford Health System
Detroit, MI
Objectives
Understand the coagulation cascade and
risks of VTE
Identify the variety of current
anticoagulants available
2012 CHEST guidelines
To bridge or not to bridge
Disclosures
Speaker’s Bureau:
GSK Pharmaceuticals
Novartis
Nursing Advisory Boards
Pfizer
Baxter
Bayer Health Care
CSL Behring
Octapharma
I have no current affiliation or financial arrangement with any
grantor or commercial interests that might have direct interest
in the subject matter of this CE program
Pathophysiology of a Thrombosis
Abnormalities of vessel wall
atherosclerosis (arterial)
trauma, erosion
deficient fibrinolysis, venous hypotonia
(pregnancy)
Abnormalities of blood flow
hypertension, turbulence
hyper-viscosity
stasis, deficient clearance of coagulation
factors
Abnormalities of blood
quantitative platelet abnormalities
thrombocytosis
decrease of inhibitors, activation of
coagulation hypercoagulability
Protein C Def, Protein S Def, Antithrombin III
Def
Vessel wall
Virchow’s Triad
Statistics
Incidence of Venous Thromboembolism exceeds 1
per 1000 cases
Over 200,000 cases reported annually in the USA
30% pts die within 30 days of diagnosis
1/5th pts sudden death due to PE
30% survive to develop recurrent VTE within 10 yrs
- greatest risk in 1st yr (5-15%) then 1%/yr
28% of cases develop venous stasis syndrome
within 20 yrs
Heit et al, 2001
Incidence increases with age from 1:1,000
people/year to 1%/year in old age
Rosendal,1999
Padua Prediction Score Risk
8 fold risk of VTE
50-75% of VTE
events in hospitalized
medical pts
Hi Risk > 4
Spyropoulos et al. Chest 2011
Heit et al. Arch In Med, 2000
Heit et al. Arch Int Med, 2002
Why Anticoagulate?
Thrombosis
Arterial
Venous
Stroke
Ineffective management with antiplatelet
medications
Atrial Fibrillation
Cardiomyopathy
Prosthetic valves
Prophylaxis during cancer therapy
Reproduced with permission from: Rao. Am J Med Sci
1998;316:69.
How Does Blood Clot - Overview
History of Anticoagulants
Coumadin© (Warfarin)
Advantages:
Disadvantages:
Inhibits production of Vit K
needed for production of
thrombin, factors II, VII, IX, X,
protein C & S
No ceiling to dosing
Monitored by INR; 2-3.0 (normal
range 0.8-1.2)
Dosing amount can decrease
with age
Inexpensive- 5 mg tabs, #30 =
$22.00
Easy to reverse;
vitamin K
Requires regular blood test
monitoring
Interactions with multiple
medications
Can be affected by oral vitamin K
food intake
Bleeding risk 1%/year long term
use
Can be difficult to regulate
Can cause tissue necrosis if
used without concomitant
heparin initially after
thrombosis
Botanicals with Potential Anticoagulant &
Interactive Effects with Coumadin©*
Alfalfa
Dong Quai
Arnica
ASA
Boldo
Bucho
Cassia
Celery
Dandelion
Fenugreek
Horseradish
Licorice
Nettle
Parsley
Prickly Ash
Quassia
Woodruff
Tonka Beans
Wild Carrot
Wild Lettuce
Sweet CloverSweet
Aniseed
Bogbean
Capsicum
Chamomile
Horse Chestnut
Meadowsweet
Passion Flower
Red Clover
Bladder Wrack
Foetida
*Non-exhaustive list
ALWAYS check formulary
Botanicals than contain Salicylates or
Antiplatelet Properties
Agrimony
Aloe Gel
Black Cohosh
Black Haw
Cassia
Clove
Feverfew
Garlic
Gingo Biloba
Ginseng
Meadowsweet Policosanol
Poplar
Senega
Willow
Wintergreen
German Sarsaparilla
Aspen
Bogbean
Dandelion
Ginger
Licorice
Onion
Tamarind
Botanicals with Coagulant
Properties
Agrimony
Goldenseal
Mistletoe
Yarrow
Affected by warfarin
Injectable Anticoagulants
Enoxaparin (Lovenox©) - LMWH
1 mg/kg Q12,
1.5 mg/kg/day
Dalteparin (Fragmin©) - LMWH
200 IU/kg daily
Tinzaparin (Innohep©) - LMWH
175 units/kg/day
Fondaparinux (Arixtra©) - Direct Anti Xa inhibitor
7.5 mg, sq daily
5.0 mg for < 50 kg
10 mg > 100 kg
Renal Dosing
Injectable Anticoagulant Properties
Advantages:
Predictable pharmacokinetic
properties and drug interactions
Can be effective in recurrent VTE
while on warfarin
Poor GI absorption not a concern
Therapeutic dosage based on
patient’s weight
Lab monitoring not routinely
needed
Rapid onset of action and
predictable clearance
convenient for frequent
interruptions due to procedures
Disadvantages:
Cost
Must perform sq injection
Difficult to use for patients with
decreased GFR
Many medical personnel do not
understand pharmacokinetics
Injectable anticoagulants
Anticoagulant
½ life
Measurement
Lovenox (Enoxaparin©)
12 hours
Heparin x assay – 4 hours post
injection
Fragmin (Dalteparin©)
19 hours
Heparin x assay– 4 hours post
injection
Innohep (Tinzaparin©)
19 hours
Heparin x assay– 4 hours post
injection
Arixtra (Fondaparinux©)
19 hours
Arixtra drug trough levels – just
prior to next dose
**All injectables are cleared through the renal
system
Affected by UFH
Low molecular
weight heparins
Direct Factor Xa
Inhibitor (Arixtra)
New Oral Anticoagulants
Rivaroxaban --- Xarelto©
Affects Xa
Hip and knee prophylaxis of DVT
Stroke in NVAF
November 2, 2012 treatment of DVT/PE
Apixaban --- Eliquis©
Affects Xa
FDA December 2012 to decrease the number of stokes and
dangerous blood clots in NVAF
Dabigatran --- Pradaxa©
Direct Thrombin inhibitor: affects IIa
FDA October 10, 2010 approval
Stroke prevention in NVAF
Pharmacology
Characteristic
Warfarin©
Rivaroxaban
Apixaban ©
Dabigatran ©
Target
Vitamin K
factors
Factor Xa
Factor Xa
Thrombin
Bioavailability
100%
60-80%
60%
6%
Dosing
OD
OD (BID)
BID
BID (OD)
Time to peak
effect
4-5 day
2-4 hours
1-2 hours
1-3 hours
Half life
40 hours
7-11 hours
12 hours
8-15 hours
Renal
clearance
None
33%
25%
80%
Monitoring
Yes
No
No
No
Interactions
Multiple
3A4/P-gp
3A4/P-gp
P-gp
©
Oral direct thrombin inhibitors
Advantages
Disadvantages
½ life of 19 hours
Oral medication
No need for blood testing
Side effects: GI upset, diarrhea,
Renal clearance of the drug
monitor renal/liver function
Drug-drug interactions
No reversal drug
Prothrombin complex concentrates
(PCC)
Feiba©; Bebulin©, Profilnine ©;
FFP, Factor VIIa;
Dialysis
Lack of understanding mechanism
Direct thrombin
inhibitors: Arixtra (sq)
Dabigatran(PO)
Direct Factor Xa
Inhibitor: Apixaban
Rivaroxaban
CHEST
Guidelines
2012
ACCP Guidelines: Chest 2012
Patients on vitamin K antagonists
(warfarin) undergoing minor dental
procedures:
Continuation of warfarin around the time of
procedure
Co-administration of oral pro-hemostatic
agents
[Grade 1C]
ACCP Guidelines: 2012
Patients who require a temporary interruption
of a warfarin before surgery and require a
normal INR for surgery:
Stop warfarin 5 days before procedure (1B)
Use of LMWH with last dose 24 hr before
surgery at ½ recommended dose (1C)
Resume warfarin 12 – 24 hours after surgery
(1C)
Resume LMWH 24 hr after procedure (1C)
ACCP Guidelines: 2012
Mechanical heart valve or atrial fibrillation
or current VTE
High risk for recurrent VTE;
Bridging with therapeutic LMWH of IV UFH
Low risk for recurrent VTE:
Low dose LMWH or no bridging with LMWH/UFH
[Grade 2C]
ACCP Guidelines: 2012
Bare metal coronary stent who require surgery
within 6 weeks of stent placement:
Continuation of ASA and clopidogrel in the perioperative period
Drug-eluting coronary stent who require
surgery within 12 months of stent placement:
Continuation of ASA and clopidogrel in the perioperative period
[Grade 2C]
ACCP Guidelines: 2012
Patients who require temporary
interruption of ASA or clopidogrel before
surgery:
Stop 7-10 days before procedure
Resume agents 24 hours after procedure
(2C)
CHADS score
Indication: Assess risk of stroke with AFib
Criteria
A. Congestive Heat Failure (1point)
B. Hypertension (1 point)
C. Age > 75 years (1 point)
D. Diabetes (1 point)
E. Stroke or TIA history (2 points)
Recommendations:
CHADS score > 2, consider bridging if on warfarin
Gage. Circulation 2004
Bridge Therapy
“Shift from oral, long-acting anticoagulants
to parenteral, short-acting anticoagulants
during sub-therapeutic levels of oral
anticoagulant in the perioperative period”
Spyropoulos et al. (2004)
Bridging Therapy
Advantages
Provides continued anticoagulation
Minimal window without anticoagulation
Cost savings for hospitalizations: ~ >$13,000
Disadvantages
Use of LMWH for 8-10 days, SQ self injection
Plan ahead
Prior insurance authorization may be needed
Requires coordination of care
Can be costly (approx. cost 10 syringes =$600$1,000)
Bridging Therapy Process Steps: Lovenox©
1.
2.
3.
4.
5.
6.
7.
8.
Hold warfarin 5 days prior to procedure
Start LMWH q12h, 4 days prior to procedure
Check INR/Platelet level day before procedure
Lovenox dose day before procedure in am ½ the
usual dose; Hold LMWH night before procedure
Restart both warfarin and LMWH q12-24 hr
hours after procedure provided there are no signs of
bleeding
Check INR on the 4th day - goal of INR > 2.0
Stop LMWH when INR >2.0
Expect to be on LMWH for 8-10 days
Bridging Therapy Process Steps:
Using longer ½ life injectables (Arixtra©)
1.
2.
3.
4.
5.
6.
7.
8.
Hold coumadin 5 days prior to procedure
Start injectable daily sq, 4 days prior to procedure
Last dose of injectable 2 days prior to event (3 ½
lives of the drug)
Check INR/Platelet level day before procedure
Restart both warfarin and injectable anticoagulant
q12-24 hr hours after procedure provided there are
no signs of bleeding
Check INR on the 4th day - goal of INR > 2.0
Stop injectable anticoagulant when INR >2.0
Expect to be on injectable anticoagulant for 8-10 days
Procedure
Date
Injectable
anticoagulant
Anticoagulated
5 days
~4-5 days
Warfarin
Normal Coagulation
Check INR
Platelet ct
Coumadin© induced tissue necrosis
Re-initiation of Coumadin©
Coumadin© causes decrease of Protein C & S
as part of the coagulation system when
initially started
potentially allows coagulation cascade to go
unchecked with increased formulation of thrombin
Onset of thrombosis also causes decreases in
Protein C & S
RESULT: Increases risk of thrombosis
Bridging process: oral agents
Xarelto©, Pradaxa©
Hold 48 hours prior to procedure
Restart 12-24 hours after procedure
Procedure
Date
1 day
Anticoagulated
2 days
Oral direct
thrombin
Normal Coagulation
Challenges
Injectables are now generic
Less availability for support programs & educational materials
Still costly
Insurance approvals
Injectables
New agents
Lack of understanding
Medications
Testing
Interactions
Bridging
Summary
Review risk/benefit of holding any form of
anticoagulation
Thrombosis vs bleeding risk
Individualized treatment
Co-ordination of care with:
Patients &/or family caregivers
Hematology; HTC
Anticoagulation clinic
Primary physician
Monitor patient during process
Check INR (as indicated)
Bleeding/bruising
Platelet count (as indicated)
Question #1
Patient is on warfarin for atrial fibrillation
Need to extract one tooth
Should warfarin be held?
Questions to ask…..
CHADS score; if high, should not stop warfarin
What is latest INR testing?; must be between 2-3
Nature of the procedure…. Increased risks?
Question #2
Patient is taking Lovenox© every 12
hours for history of pulmonary embolus
History of active colon cancer receiving
chemotherapy
Pt requires port placement
Questions to ask….
Should lovenox be held?
How?
Question #3
Patient is on Pradaxa© for atrial fibrillation
Requires 5 teeth extracted
Questions to ask….
CHADS score? Increased risk of VTE?
Amount of bleeding?
½ life of the medication
Stop Pradaxa© 2 days prior to procedure
Restart 12-24 hours after the procedure
NO injectable anticoagulant needed
Question #4
Pt on long term Arixtra© for history of recurrent
VTE
Pt history of recurrent VTE on therapeutic
warfarin
Allergy to Lovenox© itching, rash
Needs colonoscopy for Hx of polyps
Questions to ask?
Hold Arixtra©?
How?
Angela Lambing, MSN, NP-C
Hemophilia & Thrombosis
Treatment Center
Henry Ford Health System
[email protected]
313-916-9094