aticoagulation deck 2

Question 1

Factor Xa Inhibitor Oral Anticoagulants

and Direct Thrombin Inhibitor (DOACs) MOA

Answer 1

Prevent factor Xa from converting prothrombin to thrombin by binding directly to factor Xa*

Question 2

Direct Thrombin inhibitor: inhibits

Answer 2

thrombus

◦ dabigatran

Question 3

Factor Xa Inhibitor Oral Anticoagulants

and Direct Thrombin Inhibitor (DOACs) indications

Answer 3

◦ Reduction of risk of stroke and systemic embolism in nonvalvular atrial fibrillation
◦ Prophylaxis of DVT following knee replacement surgery
◦ Treatment of DVT and PE

Question 4

Factor Xa Inhibitor Oral Anticoagulants

and Direct Thrombin Inhibitor (DOACs) pharmacodynamics

Answer 4

◦ Half life variable by agent: 5-15 hours
◦ Variable renal elimination by agent
◦ Edoxaban, Rivaroxaban renal precautions
◦ Dabigatran renal contraindications

Question 5

Factor Xa inhibitors and interacting drugs

Answer 5

◦ Betrixaban and P-glycoprotein (P-gp) inhibitors
◦ Edoxaban and P-glycoprotein (P-gp) inhibitors
◦ Apixaban and P-gp or CYP3A4 inhibitors
◦ Rivaroxaban and P-gp/CYP3A4 inducers
◦ Vorapaxar and CYP3A inhibitors
◦ All: platelet inhibitors, anticoagulants, antithrombotics

Question 6

Direct Thrombin Inhibitors and interacting drugs

Answer 6

◦ Dabigatran and P-glycoprotein (P-gp) inhibitors, Rifampin, Dronedarone

Question 7

Dabigatran do not use if

Answer 7

GFR is low

Question 8

Factor Xa/Direct Thrombin Inhibitors:

Drug Interactions and ADRs

Answer 8

◦ Bleeding and Anemia
◦ Variable renal elimination: Dabigatran, edoxaban require renal adjustment
◦ Monitor renal status
◦ GI: Dyspepsia, nausea, upper abdominal pain, GI hemorrhage, diarrhea
◦ Dabigatran: Black Box warning potential for rebound thrombotic event on discontinuation

Question 9

◦ Dabigatran: Black Box warning

Answer 9

warning potential for rebound thrombotic event on discontinuation

Question 10

American College of Clinical Pharmacy (ACCP) guidelines for

Answer 10

r DVT or PE after initial

stabilization:

Question 11

DVT and PE treatment after stabalization

Answer 11

3 months of dabigatron, rivaroxaban, apixaban or endoxaban (fixed doses) for
3 months

Question 12

Factor Xa Inhibitors/Direct Thrombin Inhibitors

Answer 12

Do not require routine monitoring, if do, aPTT not INR

Question 13

Factor Xa Inhibitors/Direct Thrombin Inhibitors not used

Answer 13

Not used in pregnancy or if CrCl <15mL/min3

Question 14

◦ Idarucizumab received FDA approval in 2017 as a reversal agent for

Answer 14

dabigatran

Question 15

Andexanet alfa is an inactive, decoy

Answer 15

factor Xa (FXa) molecule that binds FXa inhibitors,
and ciraparantag is a synthetic molecule designed to bind fractionated and unfractionated
heparins, and each of the currently approved DOACs; not FDA approved

Question 16

risk of inctracranal bleeding was reduced with ___ compared with warfarn

Answer 16

DOACs

Question 17

DOAC pregnancy

Answer 17

Pregnancy category C*

Unknown whether excreted into breast milk

Question 18

DOAC peds

Answer 18

Safety and efficacy not established for pediatric patients

Question 19

DOAC advantages compared to warfarn

Answer 19

Absence of food interactions
Few strong drug interactions
Predictable pharmacokinetic and pharmacodynamic
profiles except renal and obesity
Rapid onset and offset of action
Short half-life
Absence of the need for laboratory monitoring
Wide therapeutic windows
Greater efficacy in AF
Lower risk of intracranial hemorrhage, except for
dabigatran

Question 20

DOAC disadvantages compared to warfarin

Answer 20

Higher cost
Limited specific antidotes
Limited experience and dosing
NOACs should not be used in patients with patients:
◦ severe renal and hepatic disease,
◦ mechanical heart valves
◦ younger than age 18 years
◦ the elderly

Question 21

Heparin MOA

Answer 21

Binds to antithrombin III and turns off activating factors that develop clots

Question 22

Heparin pharmacokinetics

Answer 22

◦ Given intravenously (IV) or subcutaneously (SC)
◦ Variable bioavailability
◦ Extensively protein bound
◦ Metabolized by liver and renally eliminated

Question 23

Heparin precautions and contraindications

Answer 23

◦ Pregnancy category C
◦ Avoid in advanced hepatic or renal disease
◦ Avoid in bleeding disorders or active bleeding

Question 24

Heparin is highly

Answer 24

protein bound so it can be desttroid in GI tract. Reason it isn’t oral

Question 25

Indications for heparin

Answer 25

DVT, PE, Acute coronary, anticoagulation

Question 26

heparin needs to be dosed

Answer 26

multiple times. due to short half life

Question 27

Heparin ADR

Answer 27

◦ May cause thrombocytopenia
◦ Life-threatening bleeding
◦ Pain at injection site (SC)

Question 28

Heparin antidote

Answer 28

◦ May cause thrombocytopenia
◦ Life-threatening bleeding
◦ Pain at injection site (SC)
◦ Antidote is protamine sulfate

Question 29

Heparin monitoring

Answer 29

◦ aPTT

◦ CBC with platelets

Question 30

Heparin interacions

Answer 30

Cephalosporins and penicillins
◦ Warfarin, antiplatelets, and thrombolytics
◦ Valproic acid
◦ Protamine sulfate is antagonist

Question 31

LMWH definition

Answer 31

Fragments of unfractionated heparin; smaller molecules than unfractionated heparin

Question 32

LMWH MOA

Answer 32

◦ Some effects on antithrombin III which complexes to thrombin and inactivates it
◦ Preferentially inhibits the activation of Factor Xa
◦ Minimal effects on thrombin (factor II) because of small size
◦ Less action on platelets than heparin

Question 33

LMWH Kinetics

Answer 33

◦ Volume of distribution varies between agents
◦ t1/2 is about 4h for all products, NOT protein bound
◦ Inconsistent bioavailability but Improved from heparin
◦ more predictable, dose-independent clearance
◦ Liver disease and renal disease may affect metabolism and elimination

Question 34

Indications for LMWH

Answer 34

DVT prophylaxis in medium and high-risk groups (surgical, orthopedic and medical patients)

Treatment of venous thromboembolism in pregnancy

Treatment of DVT and PE in nonpregnant women (those with both high and low risk of recurrence)

Treatment of STEMI (in both those undergoing percutaneous coronary intervention and those not)

Unstable angina
Prevention of clotting in extracorporeal circuits

Question 35

LMWH precautions

Answer 35

◦ Low body weight (<50kg), HTN, liver disease, PUD, malignancy

Question 36

LMWH contraindictions

Answer 36

◦ Known hypersensitivity to heparin or pork products
◦ Active bleeding or blood dyscrasias
◦ Suggested: trauma, epidural half-life, hemorrhagic disorders, peptic ulcer disease, recent cerebral
hemorrhage, severe hypertension, and recent surgery to the eye or nervous system

Question 37

LMWH dosing

Answer 37

◦ Each LMWH has its own unique dosing regimen because of relative proportions of anti-Xa to anti-IIa
activity
◦ There are differences in manufacturing, half-life, ratio of anti-Xa to anti-IIa activity, and dose
◦ they CANNOT be used interchangeably

Question 38

LMWH Monitoring

Answer 38

◦ Patient should monitor for side effects (no blood monitoring necessary, although periodic CBC, platelet,
hemocult stool sometimes recommended)
◦ Chromogenic anti-factor Xa assay is currently the gold standard for monitoring LMWH and fondaparinux
therapy

Question 39

LMWH Interactions

Answer 39

◦ Other drugs affecting anticoagulation

◦ PCNs, cephalosporins

Question 40

LMHW Adverse reactions

Answer 40

Bleeding, thrombocytopenia, elevated liver function tests

Question 41

LMWH first line

Answer 41

First line drug if antithrombotic therapy required during pregnancy

Question 42

LMWH is safe for

Answer 42

Safe for breast feeding

Question 43

LMWH betware of

Answer 43

Beware of spinal puncture with LMWHs because it can lead to paralysis

Question 44

LMWH risk for

Answer 44

Risks of osteoporosis and thrombocytopenia are less than with heparin

Question 45

LMWH not for

Answer 45

Not for thromboprophylaxis with mechanical heart valve

Question 46

Heparain Fast Facts (for comparason with LMWH)

Answer 46

Usually used in-patient
Requires monitoring via aPTT 
Dosed IV, SC 
Marked variability in anticoagulant
response
Short half life 
Highly protein bound
Risk of osteoporosis

Question 47

no spinal injections when on a DOAC due to

Answer 47

bleeding

Question 48

LMWH Fast Facts (for comparason with Heparin)

Answer 48

Can be used in or outpatient
Do not require blood monitoring
Dosed SC
More predictable anticoagulant response
Half life is 2-4 times that of heparin
Not protein bound
Less risk of osteoporosis