Chapter 34 - Anticoagulation Flashcards

Question 1

Q

What are anticoagulants used for?

Answer

A

Prevent blood clots from forming
Keep existing clots from becoming larger
They do not break down clots (like thrombolytics)

Question 2

Q

What are some indications for anticoagulants use?

Answer

A

Acute coronary syndromes (ACS)
Prevention of cardioembolic stroke
Prevention/treatment of venous thromboembolism (VTE),
which refers to deep vein thrombosis (DVT) and/or pulmonary embolism (PE)

Question 3

Q

What is the most common side effect of anticoagulants?

Answer

A

Bleeding, which can be fatal.

Anticoagulants are high-alert medications for this reason.

Question 4

Q

Clotting factors are primarily made in the:

Question 5

Q

The coagulation cascade has two pathways which lead to fibrin formation:

Answer

A

1) The contact activation pathway (or the intrinsic pathway)
2) The tissue factor pathway (or the extrinsic pathway).

Anticoagulants inhibit the coagulation cascade and prevent (or reduce) clot formation

Question 6

Q

What factors do warfarin inhibits?

Answer

A

Factors II, VII, IX and X

(1972)

Protein C & S

Question 7

Q

What drug inhibit factor Xa
2- Direct
3- Indirect

Answer

A

Direct (PO)
- RivaroXAban
- ApiXAban
- EdoXAban

Indirect (IV/SQ)
- Fondaparinux

Question 8

Q

4- What drugs are Direct Thrombin Inhibitors

Answer

A

IV - Argatroban, Bivalirudin
PO - Dabigatran

Factor II Prothrombin –> Factor IIa Thrombin

Question 9

Q

5/6)What drugs have both anti Xa and anti IIa activities?

Answer

A

1- Unfractionated Heparin
- Has equal anti Xa & anti IIa activities

2- Low molecular weight heparin
- More anti Xa than anti IIa activities

Question 10

Q

What is the function of thrombin?

Answer

A

Thrombin converts fibrinogen into fibrin

Fibrin strands crosslink to hold the clot together

Question 11

Q

When do you use Injectable and oral anticoagulants

Answer

A

Injectable anticoagulants are used for:
- ACS (Heart) and VTE (Leg) (treatment and prevention)

Oral anticoagulants are used mainly for:
- VTE (Leg) (treatment and prevention)
- Stroke (Brain) prevention in patients with (AFib)

Question 12

Q

What are the oral anticoag drugs?

Answer

A

1- Warfarin (Vitamin K antagonists)

DOAC: Direct acting oral anticoagulants:
2- Factor Xa inhibitors
- Rivaroxaban (Xarelto)
- Apixaban (Eliquis)
- Edoxaban

3- Thrombin Inhibitors
- Dabigatran (Pradaxa)

–> Treat/ Prevent blood clots in veins
–> Prevent stroke in A. Fib

Question 13

Q

DOACs Vs Warfarin?
1- Benefits of DOACs over Warfarin?
2- How do you dose DOACs?
3- What do you use for stroke prevention in Afib?
4- What do you use for VTE treatment?

Answer

A

1- DOACs benefits over warfarin:
- Less drug-drug interactions
- Less or comparable bleeding
- Shorter half-life

2- DOAC dosing is based on the indication and kidney/ liver function - there is no need to adjust the dose based on the INR (as with warfarin)

3- DOACs preferred for stroke prophylaxis in AFib
■ BUT - if there is moderate-to-severe mitral stenosis or a mechanical heart valve, use WARFARIN

4- Use DOACs for VTE treatment
■ BUT - if the patient has CANCER, use LMWH
■ BUT - if the patient has ANTIPHOSPHOLIPID syndrome, use WARFARIN

Question 14

Q

VITAMIN K ANTAGONISM (Warfarin)
1- Function of vitamin K
2- What happens if we antagonize Vitamin K
3- What should you watch for while on warfarin

Answer

A

1- Vitamin K is required for the carboxylation (activation) of clotting factors II, VII, IX and X

2- Without adequate vitamin K, the liver produces the clotting factors, but they have reduced coagulant activity.

3- Warfarin has a narrow therapeutic range and requires careful monitoring of the international normalized ratio (INR), which is affected by many drugs and changes in dietary vitamin K.

Question 15

Q

1- What is the function of antithrombin?

2- What drugs work on antithrombin? What do they do?

3- What drugs inhibit Factor Xa directly?

4- What should you monitor for efficacy?

Answer

A

1- Antithrombin (AT) is one of the body’s natural anticoagulants; it inactivates:
- Thrombin (factor Ila)
- Factor Xa

2- Drugs that work by binding to AT and causing a conformational change which increases AT activity 1,000-fold:
- Unfractionated heparin (UFH) (Xa = IIa)
- Low molecular weight heparins (LMWHs) (Xa > IIa)
- Fondaparinux (Arixtra) binds to AT, resulting in selective inhibition of factor Xa.

3- Inhibit factor Xa directly
- Apixaban (Eliquis)
- Edoxaban (Savaysa)
- Rivaroxaban (Xarelto)

4- These oral medications are taken once or twice daily and require no laboratory monitoring for efficacy.

Question 16

Q

1- How do UFH & LMWH inhibit thrombin & factor Xa?

2- How do Direct thrombin inhibitors work?

3- Why are IV DTis important clinically? When are they the drug of choice?

4- Name the IV and oral DTis?

Answer

A

1- UFH and LMWH indirectly inhibit thrombin and Factor Xa through AntiThrombin binding.

2- Direct thrombin inhibitors (DTis) block thrombin directly, decreasing the amount of fibrin available for clot formation.

3- IV DTis do not cross-react with heparin-induced thrombocytopenia (HIT) antibodies.
- Once HIT develops in the hospital setting, the injectable DTI ARGATROBAN is the drug of choice.

4- Oral: Dabigatran (Pradaxa)
IV: Argatroban, Bivalirudin

Question 17

Q

How do fibrinolytics work?
When do you use fibrinolytics?

Answer

A

Fibrinolytics break down existing clots but are associated with a very high risk of bleeding.
They are used when the patient could die without rapid restoration of blood flow:
– STEMI
– Acute ischemic stroke
Drugs: Streptokinase, Alteplase, urokinase

Question 18

Q

When do you use antiplatelets?
What is DAPT?

Answer

A

Antiplatelet drugs (aspirin, clopidogrel, ticagrelor) are used mainly for:
- ACS
- Stroke/TIA prevention

Dual antiplatelet therapy (DAPT) refers to using both aspirin and a P2Y12 inhibitor (e.g., clopidogrel) together, which is very common in patients who have had an ACS.
Antiplatelet drugs are NOT sufficient for treating DVT/PE.

Question 19

Q

When are oral anticoags used?

Answer

A

Oral anticoagulants are used mainly in AFib (for stroke prevention) and for DVT/PE (treatment and prevention).
Oral medications like Xarelto or Eliquis are not indicated for ACS when platelet aggregation is the main target of drug therapy.

Question 20

Q

An acute drop in hemoglobin (>= … g/dL) could signify that bleeding is occurring (visible or not).

Question 21

Q

What could be some causes of epistaxis?

Answer

A

1) Epistaxis: From drugs, dry nasal mucosa (esp. with dry heat), nose-blowing

Question 22

Q

What could be some causes of gum bleeds?

Answer

A

2) Gums: New, or worse than usual from gingivitis, drugs

Question 23

Q

What could be some causes of bruising?

Answer

A

From drugs (chronic steroids)
Thrombocytopenia/clotting disorder
Cushing’s syndrome
Malnutrition
Physical abuse
Fracture/sprain
Infection

Question 24

Q

What could be some causes of hematoma?

Answer

A

From drugs
On abdomen from LMWH injection that was rubbed (do not rub!)
An epidural or spinal hematoma in a patient using a LMWH or DOAC who is given neuraxial anesthesia
Spinal puncture

Question 25

Q

What could be some causes of emesis?

Answer

A

■ Coffee-ground emesis (vomit)- from bleeding in upper GI tract
■ Esophageal chronic reflux (esophagitis, Barrett’s)
■ Stomach From ulcer (NSADI-induced)
■ Duodenal From ulcer (H. pylori-induced)

Question 26

Q

What could be some causes of hematuria?

Answer

A

From UTls
Kidney stones (calculi)
Prostatitis
Kidney disease

Question 27

Q

What could be some causes of bleeding from anus?

Answer

A

Light red: from hemorrhoids, rectal tear
Black and “tarry” (sticky), smelly stool: from esophagus, stomach (NSAID-induced) or duodenum (H.pylori-induced)
Other causes of rectal bleeding:
. Diverticulosis
. Colon cancer
. IBD (Crohn’s, ulcerative colitis)
. Colon polyps (benign or cancerous)
–> Rectal bleeding from polyps can be occult (not visible, requires tests (FOBT) to identify)
Bloody diarrhea (dysentery}- from infection (C.difficile, Shigella, Entamoeba histolytica)

Question 28

Q

Drugs that cause bleeding include:

Answer

A

Anticoagulants
Antiplatelets
NSAIDs
Natural products (ginkgo/SSRls, SNRls increase bleeding risk.

Question 29

Q

How does UFH work?

Answer

A

UFH binds to antithrombin (AT)
Which then inactivates thrombin (factor Ila) and factor Xa (as well as factors IXa, Xla, Xlla and plasmin)
And prevents the conversion of fibrinogen to fibrin

Question 30

Q

Unfractionated Heparin:
- Indications
- Dosing

Answer

A

1) Prophylaxis of VTE: 5,000 units SC Q8-12H
2) Treatment of VTE: 80 units/kg IV bolus; 18 units/kg/hr infusion
3) Treatment of ACS/ STEMI: 60 units/kg IV bolus (max 4,000 units); 12 units/kg/hr infusion (max 1,000 units/hr)

Question 31

Q

Which weight should you use for dosing UFH?

Answer

A

Total body weight

Question 32

Q

What is the onset of action of IV and SC heparin?

Answer

A

Onset:

IV: immediate
SC: 20-30 min
– t1⁄2 =1.5 hrs

Question 33

Q

Can you give LMWH instead of heparin in HIT?

Answer

A

HIT antibodies have cross-sensitivity with LMWHs

Question 34

Q

CONTRAINDICATIONS with heparin

Answer

A

Uncontrolled active bleed (intracranial hemorrhage)
Severe thrombocytopenia
History of HIT
Hypersensitivity to pork products

Some products contain benzyl alcohol as a preservative (do not use in neonates, infants, pregnancy and breastfeeding)

Question 35

Q

Warning with heparin (Med safety)

Answer

A

Fatal medication errors:
- Verify the correct concentration is chosen

Question 36

Q

SIDE EFFECTS with heparin

Answer

A

Bleeding (Epistaxis, bruising, gingival, GI)
Thrombocytopenia
HIT
Hyperkalemia
Osteoporosis (with long-term use)
Alopecia

Question 37

Q

MONITORING with heparin

When do you suggest possible HIT?

Answer

A

aPTT or anti-Xa level:
. Check 6 hours after initiation and
. Every 6 hrs until therapeutic
. Then every 24 hrs
. With every dosage change
aPTT therapeutic range: 1.5-2.5 x control
Anti-Xa therapeutic range: 0.3-0.7 units/ml
aPTT and anti-Xa monitoring are not required for SC (prophylactic) dosing
Platelets, Hgb, Hct at baseline and daily (dec in platelets > 50% from baseline suggests possible HIT)

Question 38

Q

Antidote of Heparin

Answer

A

Protamine

Question 39

Q

When do we commonly use Heparin continuous IV infusion? Why?

Answer

A

Unpredictable anticoagulant response (has variable and extensive binding to plasma proteins and cells)
Continuous IV infusions are common for treating VTE and ACS because heparin has a very short half-life

Question 40

Q

When do you give Heparin IM?

Answer

A

Do not give IM due to hematoma risk

Question 41

Q

What is HepFlush and why do we use it?

Answer

A

Heparin lock-flushes (HepFlush) are only used to keep IV lines open.

Question 42

Q

Medication Errors with Heparin:

Answer

A

Fatal errors, especially in neonates, occurred when the incorrect heparin strength (higher dose) was chosen.
Heparin injection 10,000 units/ml and flushes 10 or 100 units/ml look and sound alike.

Question 43

Q

LMWH drugs and brand

Answer

A

Enoxaparin (Lovenox)
Dalteparin (Fragmin)

Question 44

Q

Lovenox come in different doses:
1 mg = … units antiXa activity

Answer

A

1 mg= 100 units anti-Xa activity

Question 45

Q

LMWH - Enoxaparin (Lovenox)
- Indications
- Dose

Answer

A

1) Prophylaxis of VTE: 30 mg SC Q12H or 40 mg SC daily
– CrCI < 30 ml/min: 30 mg SC daily

2) Treatment of VTE & UA/ NSTEMI
- 1 mg/kg SC Q12H or
- 1.5 mg/kg SC daily (only for inpatient VTE treatment)
– CrCI < 30 ml/min: 1 mg/kg SQ daily
– Use total body weight for dosing

3) Treatment of STEMI
- Patients < 75 years: 30 mg IV bolus plus 1 mg/kg SC dose followed by 1 mg/kg SC Q12H
– CrCI < 30 ml/min: 30 mg IV bolus plus 1 mg/kg SC dose followed by 1 mg/kg SC daily
- Patients >= 75 years: 0.75 mg/kg SC Q12H (no bolus)
– CrCI < 30 ml/min: 1 mg/kg SC daily (no bolus)

Question 46

Q

LMWH - Dalteparin
- Brand
- Indication

Answer

A

Fragmin
Prophylaxis of VTE: 2,500 - 5,000 units SC daily
Treatment of UA/NSTEMI: 120 units/kg (max 10,000 units) SC Q12H

Question 47

Q

LMWH BBW

Answer

A

Patients receiving neuraxial anesthesia (epidural, spinal) or
Undergoing spinal puncture

–> Are at risk of hematomas and subsequent paralysis

Question 48

Q

LMWH CI

Answer

A

History of HIT
Active major bleed
Hypersensitivity to pork

Question 49

Q

LMWH SE

Answer

A

Bleeding
Anemia
Injection site reactions (pain, bruising, hematomas)
Dec platelets (thrombocytopenia, including HIT)

Question 50

Q

LMWH monitoring

Answer

A

Platelets, Hgb, Hct, SCr
Anti-Xa monitoring:
– No need (More predictable anticoagulant response than UFH
– Monitor in pregnancy
– Obtain peak anti-Xa levels 4 hours post SC dose
Monitoring may be done in obesity, low body weight, pediatrics, elderly or renal insufficiency
aPTT is not used
– It measures how long it takes for your blood to form a clot

Question 51

Q

Antidote of lmwh?
Should you expel air bubble from syringe?
When do you administer IM?
Where should you store it?

Answer

A

Antidote: protamine
Do not expel air bubble from syringe prior to injection (can cause loss of drug)
Do not administer IM
Store at room temperature

Question 52

Q

UFH/LMWH Drug Interactions

Answer

A

Other anticoagulants
Anti platelet drugs
Some herbal supplements
NSAIDs, SSRIs, SNRls
Thrombolytics

Question 53

Q

HEPARIN-INDUCED THROMBOCYTOPENIA:
- What is HIT
- It has a high risk for:
- What happens if left untreated?
- What is HITT and what can it cause?
- Whats the estimated incidence of HIT?
- What is the typical onset of HIT?
- How do you diagnose it?
- What is the most common sign of HIT?

Answer

A

An immune-mediated IgG drug reaction
Has a high risk of venous and arterial thrombosis.
The immune system forms antibodies against heparin bound to platelet factor 4 (PF4), the antibodies then join with heparin and PF4 to create a complex, and this complex binds to the Fc receptors on platelets.
This causes platelet activation and a release of pro-coagulant microparticles.
If left untreated, HIT can lead to a prothrombotic state causing many complications including heparin-induced thrombocytopenia (most common sign of HIT) and thrombosis (HITT).
HITT leads to amputations, post-thrombotic syndrome and/or death.
The estimated incidence of HIT is -3% of patients exposed to heparin for more than four days.
It is lower with a shorter duration of treatment.
The typical onset of HIT occurs 5 - 14 days after the start of heparin or within hours if a patient has been exposed to heparin within the past 3 months.
A diagnosis is made by:
– A compatible clinical picture
– An unexplained drop in platelet count (defined as > 50% drop from baseline) and
– Laboratory confirmation of antibodies (ELISA test and confirmatory serotonin release assay) or
– Platelet activation by heparin

Question 54

Q

MANAGEMENT OF HIT COMPLICATED BY THROMBOSIS (HITT)

1) What should you do if HIT was suspected

2) What should you do if the pt is on warfarin and got diagnosed with HIT?

3) What anticoagulant is recommended for pts with HIT?

4) When can you start warfarin therapy?

5) At what dose should you start warfarin?

6) Should you overlap with another anticoag?

7) Do other anticoags increase INR?

8) What anticoag is preferred if urgent cardiac surgery or PCI is required?

Answer

A

1) Stop all forms of heparin and LMWH including heparin flushes and heparin-coated catheters.

2) Stop warfarin & Give vitamin K
– Although the patient is at a high risk of thrombosis, warfarin use with a low platelet count has a high correlation with warfarin-induced limb gangrene and necrosis.

3) Non-heparin anticoagulants (in particular, Argatroban) over heparin, LMWH or vitamin K antagonists.

4) Do not start warfarin therapy until the platelets have recovered to > 150,000/mm3

5) Warfarin should be initiated at lower doses (5 mg maximum).

6) Overlap warfarin with a non-heparin anticoagulant for a minimum of five days and until the INR is within target range for 24 hours.

7) Argatroban can increase the INR; the value must be interpreted cautiously.

8) If urgent cardiac surgery or PCI is required, bivalirudin is the preferred anticoagulant.

Question 55

Q

FACTOR Xa INHIBITORS drugs and brands

Answer

A

Direct - PO:
- Apixaban (Eliquis)
- Edoxaban (Savaysa)
- Rivaroxaban (Xarelto)

Indirect inhibitor of factor Xa (Inj):
- Fondaparinux (Arixtra)
– Injectable synthetic pentasaccharide
– Selectively inhibits factor Xa via antithrombin (AT)
– Used off-label for HIT

Question 56

Q

Eliquis DVT/PE Starter Pack:
What should the pt do if they missed a dose?

Answer

A

Eliquis DVT/PE Starter Pack: 30-day blister pack

Usual dose: 10 mg PO BID x 7 days, then 5mg PO BID

Missed Dose:
- Take immediately on the same day
- Then twice daily administration should be resumed
- The dose should not be doubled to make up for a missed dose

Question 57

Q

Factor Xa Inh - Apixaban (Eliquis)
- Indication
- Dose

Answer

A

1) Nonvalvular AFib (stroke prophylaxis): 5 mg PO BID
2.5 mg BID IF 2 of the following are present:
- Age >= 80 years
- Weight <= 60 kg
- SCr >= 1.5 mg/dl

2) Treatment of DVT/PE: 10 mg PO BID x 7days then 5 mg PO BID

3) Prophylaxis for DVT: 2.5 mg PO BlD
– For 12 days after knee replacement surgery
– For 35 days after hip replacement surgery
- Give first dose 12-24 hours after surgery

4) Reduction in the Risk of Recurrence of DVT/PE: 2.5 mg PO BID after at least 6 months of treatment for DVT/PE

Question 58

Q

Rivaroxaban (Xarelto)

Xarelto Starter Pack:
What should the pt do if they missed a dose?

Answer

A

30-day blister pack containing 15 mg and 20 mg tablets (for ease of prescribing for DVT/PE treatment)

Missed Dose: Take as soon as possible on the same day as follows:

If taking 15 mg twice daily:
– Take immediately to ensure intake of 30 mg/day (in this particular instance, two 15 mg tablets may be taken at once);
– Then resume regular schedule on the following day
If taking 10, 15 or 20 mg once daily:
– Take immediately on the same day; otherwise skip

Question 59

Q

Factor Xa inh - Rivaroxaban (Xarelto)
- Indications
- Dose

Answer

A

1) Nonvalvular AFib (stroke prophylaxis) (Ens)
- CrCI > 50 ml/min: 20 mg PO daily WITH EVENING MEAL
- CrCI 15-50 ml/min: 15 mg PO daily WITH EVENING MEAL
- CrCI < 15 ml/min: avoid use

2) Treatment of DVT/PE (To know)
- 15 mg PO BID x 21 days then 20 mg PO daily with food
– CrCI < 30 ml/min: avoid use

3) Prophylaxis for DVT (after knee/hip replacement) (Ens)
- 10 mg PO daily (for 12 days after knee or 35 days after hip replacement surgery);
- Give first dose 6-10 hours after surgery
- CrCI < 30 ml/min: avoid use

4) Reduction in the Risk of Recurrence of DVT and PE (Ens)
- 10 mg PO daily after at least 6 months of standard treatment
- CrCI < 30 ml/min: avoid use

5) Reduction in the Risk of Major CVD Events in CAD/PAD (Ens): 2.5 mg PO BID in combination with low-dose aspirin
– CrCI < 15 ml/min: avoid use

6) Prophylaxis of VTE in Acutely ill Medical Patients (Ens): 10 mg PO daily for a duration of 31 to 39 days
– CrCI < 30 ml/min: avoid use

Doses >=15 mg must be taken with food;
10 mg dose can be taken without regard to meals

Question 60

Q

Xarelto doses with or without food?

Answer

A

> = 15 mg must be taken with food;
10 mg dose can be taken without regard to meals

Question 61

Q

Edoxaban (Savaysa) Tablet - Missed Dose:

Answer

A

Take immediately on the same day; the dose should not be doubled to make up for a missed dose

Question 62

Q

Edoxaban (Savayas)
- Indication
- Warnings

Answer

A

Nonvalvular AFib (stroke prophylaxis):
CrCI > 95 ml/min: do not use (to know)

(Ens)
- CrCI 51-95 ml/min: 60 mg daily
- CrCI 15-50 ml/min: 30 mg daily
- CrCI < 15 ml/min: not recommended

2) Treatment of DVT/PE
- 60 mg daily
- Start after 5-10 days of parenteral anticoagulation (To know)

(Ens)
- CrCI 15-50 ml/min, body weight <= 60 kg or on certain P-gp inhibitors: 30 mg daily
- CrCI < 15 ml/min: not recommended

Question 63

Q

BBW: Oral direct factor Xa inhibitor

Answer

A

All:
– Patients receiving neuraxial anesthesia (epidural, spinal) or
– Undergoing spinal puncture are at risk of hematomas and subsequent paralysis
Apixaban, edoxaban and rivaroxaban: premature discontinuation inc risk of thrombotic events
Edoxaban only: reduced efficacy in non valvular AFib patients with CrCI > 95 ml/min; do not use

Question 64

Q

CI of Oral direct factor Xa inhibitor

Answer

A

Active pathological bleeding

Answer 63

A

Not recommended with:
- Prosthetic heart valves or
- Antiphospholipid syndrome

Avoid in patients with:
- Moderate to severe hepatic impairment

Answer 64

A

Generally well-tolerated, unless bleeding occurs

Edoxaban: rash, inc LFTs

Answer 65

A

Hgb, Hct, SCr, LFTs
No monitoring of efficacy required

Answer 66

A

1) Andexanet alfa (Andexxa)

2) Can be crushed and put on applesauce; crushed and mixed in water, D5W or apple juice or suspended in water to administer by NG tube

3) Betrixaban is no longer available in the U.S.

Answer 67

A

Discontinue 24 hours prior to elective surgery (rivaroxaban, edoxaban)
Discontinue 48 hours prior to elective surgery with moderate-high bleeding risk or 24 hours prior with a low bleeding risk (apixaban)

Answer 68

A

Arixtra
Injectable Indirect Factor Xa Inhibitor (SC)

Answer 69

A

1) Prophylaxis of VTE
>=50 kg: 2.5 mg SC daily
< 50 kg: contraindicated

2) Treatmentof VTE
< 50 kg: 5 mg SC daily
50-100 kg: 7.5 mg SC daily
> 100 kg: 10 mg SC daily

Both Indications
CrCI 30-50 ml/min: use caution

Answer 70

A

Patients receiving neuraxial anesthesia (epidural, spinal) or undergoing spinal puncture are at risk of hematomas and subsequent paralysis

Answer 71

A

Severe renal impairment (CrCI< 30 ml/min)
Active major bleed
Bacterial endocarditis
Thrombocytopenia with positive test for anti-platelet antibodies in presence of fondaparinux

Answer 72

A

Bleeding (Epistaxis, bruising, gingival, GI)
Anemia
Local injection site reactions (rash, pruritus, bruising)
Thrombocytopenia
Hypokalemia
Hypotension

Answer 73

A

Anti-Xa levels (3 hrs post-dose)
Platelets
Hgb
Hct
SCr

Answer 74

A

Do not expel air bubble from syringe prior to injection
No antidote
Do not administer IM

Answer 75

A

1) Other anticoagulants (Avoid)
– Monitor for antiplatelet drugs, some herbals, NSAIDs, SSRis, SNRis, thrombolytics

2) Apixaban is a substrate of CYP450 3A4 (major) and P-gp.
– Avoid use with inducers of CYP3A4 and P-gp (carbamazepine, phenytoin, rifampin, St. John’s wort).

3) Rivaroxaban is a substrate of CYP3A4 (major) and P-gp.
- Avoid use with drugs that are combined P-gp and strong CYP3A4 inducers
or combined P-gp and strong CYP3A4 inhibitors (ketoconazole, itraconazole, lopinavir/ritonavir, ritonavir, conivaptan).

4) Edoxaban is a substrate of P-gp; avoid use with rifampin.
- When treating DVT/PE, reduce dose to 30 mg daily with verapamil, macrolides (azithromycin, clarithromycin, erythromycin) and oral itraconazole or ketoconazole.

5) Cobicistat (Tybost), Stribild and Genvoya (each containing cobicistat) can increase exposure to the factor Xa inhibitors.
- Rivaroxaban should not be used with any of these medications.

Answer 76

A

Rivaroxaban when INR is < 3
Edoxaban when INR is <= 2.5
Apixaban when INR is < 2
Dabigatran when INR is < 2

(Remember: READ)

Answer 77

A

Overlap Xa inhibitor with warfarin until INR therapeutic
Stop Xa inhibitor
Start parenteral anticoagulant and warfarin at next scheduled dose

https://tam.nhsh.scot/healthcare-professional-information/therapeutic-guidelines/cardiovascular/anticoagulation/anticoagulant-switching/

Answer 78

A

Start warfarin 1-3 days before stopping dabigatran (determined by renal function).

Answer 79

A

Directly inhibit thrombin (factor Ila);
Bind to the active thrombin site of free and clot-associated thrombin.

Answer 80

A

Pradaxa
Oral Direct Thrombin Inhibitor

Missed Dose:
- Take immediately unless it is within 6 hours of next scheduled dose;
- The dose should not be doubled to make up for a missed dose

Answer 81

A

150 mg BID
- CrCI 15-30 ml/min: 75 mg BID
- CrCI<15ml/min: avoid use

Answer 82

A

150 mg BID
To know: start after 5-10 days of parenteral anticoagulation
CrCI <= 30 ml/min: avoid use

Answer 83

A

110 mg on day 1, then 220 mg daily
CrCI <= 30 ml/min: avoid use

Answer 84

A

Patients receiving neuraxial anesthesia (epidural, spinal) or undergoing spinal puncture are at risk of hematomas and subsequent paralysis
Premature discontinuation inc risk of thrombotic events

Answer 85

A

Active pathological bleeding
Treatment of patients with mechanical prosthetic heart valves

Answer 86

A

Antiphospholipid syndrome

Answer 87

A

Dyspepsia, gastritis-like symptoms, bleeding (including more GI bleeding)

Answer 88

A

Hgb, Hct, SCr
No monitoring of efficacy required

Answer 89

A

Antidote: idarucizumab (Praxbind)
Protect from moisture; dispense in original container and discard 4 months after opening
Blister packs are good until the date on the pack
Swallow capsules whole (do not break, chew, crush or open); do not administer by NG tube
Can inc aPTT, PT/INR
Discontinue if undergoing invasive surgery
– 1-2 days before if CrCI >= 50 ml/min
– 3-5 days before if CrCI < 50 ml/min)

Answer 90

A

1) Argatroban
Indicated for HIT and in patients undergoing PCI who are at risk for HIT

2) Bivalirudin (Angiomax)
Indicated for patients with ACS undergoing PCI who are at risk for HIT

Answer 91

A

To know:
- Used in patients at risk for HIT
- Argatroban: dec dose in hepatic impairment
- Bivalirudin: dec dose when CrCI <30 ml/min

HIT
- CrCI <= 30 ml/min: avoid use
- Argatroban: start at 2 mcg/kg/ min, then titrate to target aPTT
- Max: 10 mcg/kg/min

PCI
- IV bolus followed by an infusion;
- All are weight-based

Answer 92

A

Argatroban & Bivalirudin

CONTRAINDICATIONS
Active major bleeding

SIDE EFFECTS
Bleeding (mild to severe), anemia

MONITORING
aPTT and/or activated clotting time (for bivalirudin), platelets, Hgb, Hct, renal function

NOTES
- Safe with history of HIT; no cross-reaction with HIT antibodies
- No antidote
- Argatroban can inc INR; if starting on warfarin concurrently, dose cautiously and do not use a loading dose of warfarin

Answer 93

A

■ Avoid using with other anticoagulants (unless benefit outweighs risk).
- Monitor for additive effects with other drugs that can inc bleeding risk (antiplatelet drugs, some herbals, NSAIDs, SSRis, SNRis, thrombolytics).

■ Dabigatran is a substrate of P-gp; avoid use with rifampin.

■ Nonvalvular AFib:
- If CrCl 30 - 50 mL/min and patient is taking P-gp inhibitors (dronedarone or systemic ketoconazole), reduce dose to 75 mg BID.
- In severe renal impairment (CrCl 15 - 30 mL/min), avoid use with any P-gp inhibitors.

■ Other indications: avoid use with P-gp inhibitors in patients with CrCl< 50 mL/min.

■ Cobicistat (Tybost) and cobicistat-containing Stribild and Genvoya can increase exposure to dabigatran.
- Recommendations depend on renal function and indication for dabigatran.

Answer 94

A

Competitively inhibits the C1 subunit of the multi-unit vitamin K epoxide reductase (VKORCl) enzyme complex.
This reduces the regeneration of vitamin K epoxide and causing depletion of active clotting factors II, VII, IX and X and proteins C and S.

Answer 95

A

Coumadin, Jantoven
Tablet
Racemic mixture of R- and S- enantiomers with the S-enantiomer being 2.7-3.8 times more potent

Missed Dose:
- Take immediately on the same day
- Do not double the dose the next day to make up for a missed dose

Answer 96

A

Healthy outpatients:
- 10 mg daily for first 2 days
- Then adjust dose per INR values

Lower doses (< 5 mg) for:
- Elderly
- Malnourished
- Taking drugs which can inc warfarin levels,
- Liver disease
- Heart failure
- Have a high risk of bleeding

Notes:
- Take at the same time each day
- Highly protein bound (99%)

Answer 97

A

BOXED WARNINGS
Major or fatal bleeding

CONTRAINDICATIONS

Pregnancy (except with mechanical heart valves at high risk for thromboembolism)
Preeclampsia/eclampsia
Possible miscarriage
Noncompliance
Hemorrhagic tendencies
Blood dyscrasias
Uncontrolled hypertension
Pericarditis or pericardial effusion
Bacterial endocarditis
Recent or potential surgery of the eye or CNS
Major regional lumbar block anesthesia or traumatic surgery resulting in large open surfaces

Answer 98

A

Tissue necrosis/gangrene
HIT (contraindicated as monotherapy in the initial treatment of active HIT)
Systemic atheroemboli and cholesterol microemboli
Presence of CYP2C9*2 or *3 alleles and/or polymorphism of VKORC1 gene may increase bleeding risk (routine genetic testing is not currently recommended)

Answer 99

A

Bleeding/bruising (mild to severe), skin necrosis, purple toe syndrome

Answer 100

A

Goal INR 2-3 (target 2.5): most indications
– VTE
– AFib
– Bioprosthetic mitral valve
– Mechanical aortic valve
– Antiphospholipid syndrome
Goal INR 2.5-3.5: high-risk indications such as
– A mechanical mitral valve
– 2 mechanical heart valves
Begin INR monitoring after the initial 2 or 3 doses, or if on a chronic, stable dose of warfarin, monitor every 4-12 weeks Hct, Hgb, signs of bleeding

Answer 101

A

vitamin K

Answer 102

A

Dental cleanings and single tooth extraction do not generally require a change in warfarin dosing, if INR is in therapeutic range

Answer 103

A

Pink (1 mg)
Lavender (2 mg)
Green (2.5 mg)
Brown/Tan (3 mg)
Blue (4 mg)
Peach (5 mg)
Teal (6 mg)
Yellow (7.5 mg)
White (10 mg)

Please Let Greg Brown Bring Peaches To Your Wedding

Answer 104

A

■ Warfarin:
- CYP2C9 (major) substrate
- CYP2C19 (minor) substrate
- CYP3A4 (minor) substrate
- Inhibitor of CYP2C9 (weak) and 2Cl9 (weak).
– Avoid use with tamoxifen.

■ CYP2C9 inducers can dec INR; these include:
- Aprepitant, bosentan, carbamazepine, phenobarbital, phenytoin, primidone, RIFAMPIN (large dec in INR), licorice and St. John’s wort.

■ CYP2C9 inhibitors can inc INR; these include:
- Amiodarone, azole antifungals (fluconazole, ketoconazole, voriconazole), capecitabine, fluvastatin, fluvoxamine, metronidazole, tigecycline, TMP/SMX and zafirlukast.
– When starting amiodarone, dec the dose of warfarin by 30-50%.

■ Other antibiotics: penicillins, including amoxicillin, some cephalosporins, quinolones and tetracyclines inc the anticoagulant effect of warfarin - monitor INR.

■ Check for CYP1A2, 2Cl9 and 3A4 interactions; these occur, but usually have less of an effect on INR.

Answer 105

A

■ NSAIDs, antiplatelet agents, other anticoagulants, SSRis and SNRis.
These interactions inc bleeding risk, but the INR may not be increased.

■ Drugs that inc clotting risk (estrogen and SERMs) should be discontinued if possible.

Answer 106

A

■ Warfarin + Natural products: Monitor the INR closely
- But some natural products contain plant salicylates (willow bark) which increase the risk of bleeding without increasing the INR.

– INC bleeding risk with warfarin:
. “the 5 G’s” (garlic, ginger, ginkgo, ginseng, glucosamine)
. Dong quai
. Vitamin E
. High doses of fish oils
. Grapefruit
. Willow bark
. Wintergreen oil

– DEC effectiveness of warfarin:
. Green tea
. Coenzyme Ql0
. St. John’s wort.
American ginseng may decrease the effects of warfarin, but there is evidence that both American and Panax ginseng inhibit platelet aggregation (listed above), which potentially has the opposite effect.

■ Any additions of vitamin K will dec the INR.
- Stay consistent with the amount of vitamin K in the diet
- Tube feeds should be held one hour before and after warfarin.

Answer 107

A

Spinach
Broccoli
Brussel sprouts
Cabbage
Beef liver
Kale
Mustard greens
Swiss chard
Collard greens
Parsley

Others: canola oil, cauliflower, chickpeas, cole slaw, coriander, endive, lettuce (red leaf or butterhead), soybean oil, some teas

Answer 108

A

In healthy outpatients, the initial starting dose of warfarin should be 10 mg daily for the first two days, then adjust per INR values.
In patients with acute DVT/PE, start warfarin on the same day as the parenteral anticoagulant (enoxaparin or UFH) and continue both anticoagulants for a minimum of 5 days and until the INR is > 2 for at least 24 hours.
Both criteria must be met.
Routine pharmacogenomic testing is not recommended.
Routine use of vitamin K supplementation is not
recommended in patients taking warfarin.
For patients with stable therapeutic INRs presenting with a single subtherapeutic (low) INR value, routinely bridging with UFH or LMWH is not recommended.
For patients with previously stable therapeutic INRs who present with a single out-of-range INR of <= 0.5 below or above the therapeutic range, continue current dose and obtain another INR within 1- 2weeks.
For patients with consistently stable INRs on warfarin therapy, INR testing can be done up to every 12 weeks rather than every 4 weeks.
Warfarin is highly protein bound. Caution is advised with other highly protein bound drugs that may displace warfarin such as phenytoin, valproic acid and others

Answer 109

A

Major adverse effect of anticoagulants: Bleeding
Life-threatening bleeding or requires surgery –> Give antidote
Protamine combines with strongly acidic heparin to form a stable salt complex, neutralizing the anticoagulant activity of UFH and LMWH.

Other drug-specific antidotes include:
- Phytonadione (vitamin K)
- Praxbind
- Andexxa

Kcentra is indicated for the urgent reversal of warfarin.
Prothrombin complex concentrates (PCCs) are sometimes used (off-label) for reversal of factor Xa inhibitors.
If PCCs are used in this manner, monitoring clotting tests (PT, PTT, INR, anti-Xa) to assess reversal is not useful and is not recommended.

Answer 110

A

Protamine sulfate

1) For IV UFH Reversal

1 mg protamine will reverse ~100 units of heparin
Since UFH has a very short half-life, reverse the amount of heparin given in the last 2-2.5 hours; max dose: 50 mg

2) For LMWH Reversal

Enoxaparin given within the last 8 hours:
1 mg protamine per 1 mg of enoxaparin (can neutralize ~60% of the anti-Xa activity of LMWH)
Enoxaparin given > 8 hours ago: 0.5 mg protamine per 1 mg of enoxaparin
Dalteparin: 1 mg protamine for each 100 anti-Xa units of dalteparin

Answer 111

A

Hypersensitivity
Hypotension
Cardiovascular collapse
Non- cardiogenic pulmonary edema
Pulmonary vasoconstriction

Answer 112

A

SIDE EFFECTS
- Hypotension
- Bradycardia
- Flushing
- Anaphylaxis

MONITORING
- aPTT
- anti-Xa levels
- cardiac monitoring {ECG, BP, HR)

NOTES
- Rapid IV infusion causes hypotension
- Administer slow IV push {50mg over 10 minutes)
- Inject without further dilution over 1-3 minutes

Answer 113

A

ldarucizumab (Praxbind)

Dose: 5 grams IV {given as 2 separate 2.5 gram doses no more than 15 minutes apart)

WARNINGS
Thromboembolic risk, risk of serious adverse reactions due to sorbitol excipient

SIDE EFFECTS
HA, dec K,delirium, constipation, fever

NOTES
Do not confuse with IDArubicin

Answer 114

A

Andexanet alfa (Andexxa)

Bolus, followed by infusion
Dosing is specific to the Xa inhibitor, the dose and when the last Xa inhibitor dose was taken

BBW:
Thromboembolic risks, ischemic events, cardiac arrest, sudden death

SIDE EFFECTS
Injection site reaction, DVT,ischemic stroke, UTI, pneumonia

NOTES
Not indicated for reversal of factor Xa inhibitors other than apixaban and rivaroxaban

Answer 115

A

Vitamin K or phytonadione (Mephyton)
IV/PO (SC route not recommended due to variable absorption; IM route not recommended due to risk of hematoma)

BBW: Hypersensitivity reactions (anaphylaxis)

SIDE EFFECTS: Anaphylaxis

NOTES: Requires light protection during administration

Answer 116

A

Antidote for warfarin reversal:
Factors: II, VII, IX, X, ProteinC, Protein S
BBW: Arterial and venous thromboembolic complications have been reported
CI: Disseminated intravascular coagulation (DIC) and known HIT (Contains heparin)
WARNINGS: Made from human blood and may carry risk of transmitting infectious agents
SIDE EFFECTS: HA, N/V/D, arthralgia, hypotension, dec K, thrombotic events

NOTES:
– Administer with vitamin K
– Do not let drug back-up into line; will clot
– Refrigerate; allow to reach room temp prior to administration
– Each vial can have a different potency of multiple coagulation factors; actual potency is stated on the vial

Answer 117

A

Antidote for warfarin reversal: (No 7)
WARNINGS
Contains factors II, IX and X but low or non therapeutic levels of factor VII and should not be confused with Kcentra, which contains therapeutic levels of factor VII
Made from human blood and may carry risk of transmitting infectious agents (e.g.,viruses)

NOTES
Slow infusion and give antihistamine to minimize side effects
Administer with vitamin K

Answer 118

A

Antidote for warfarin reversal
BOXED WARNINGS
Serious thrombotic events are associated with the use of factor VIia

Answer 119

A

Elevated INRs–> increased risk of bleeding.
Vitamin K is used to reverse warfarin; it can be used by itself or with other medications for life-threatening bleeding.
Bleeding (regardless of the INR) will warrant more serious intervention.
Oral formulations of vitamin K (generally at doses of 2.5 - 5 mg) are preferred for reversal in patients without significant or major bleeding.
Vitamin K given subcutaneously (SC) has a slow onset and a variable response; avoid SC injections.
Avoid the intramuscular (IM) route due to the risk of hematoma formation.
Intravenous vitamin K should be used only when the patient is experiencing serious bleeding.
IV injection is reported to cause anaphylaxis in 3 out of 100,000 patients, so infuse slowly.

Answer 120

A

1) INR above therapeutic range but < 4.5 without bleeding:
- Reduce or skip warfarin dose
- Monitor INR
- Resume warfarin when INR therapeutic
- Dose reduction may not be needed if only slightly above therapeutic range

2) Supratherapeutic INR of 4.5-10 without bleeding
- Routine use of vitamin K is not recommended if no evidence of bleeding
- Hold 1-2 doses of warfarin
- Monitor INR
- Resume warfarin at lower dose when INR therapeutic
- Vitamin K can be used if urgent surgery needed (<= 5 mg, with additional 1-2 mg in 24 hours if needed) or bleeding risk is high (1- 2.5 mg)

3) INR > 10 without bleeding
- Hold warfarin
- Give oral vitamin K 2.5-5 mg even if not bleeding
- Monitor INR
- Resume warfarin at a lower dose when INR is therapeutic

4) Major bleeding
- Hold warfarin
- Give vitamin K 5-10 mg by slow IV injection and four-factor prothrombin complex concentrate (PCC)
- PCC suggested over fresh frozen plasma (FFP) due to risks of allergic reactions, infection transmission, longer preparation time, slower onset and higher volume.

Answer 121

A

■ Stop warfarin therapy approximately 5 days before major surgery.

In patients with a mechanical heart valve, AFib or VTE at high risk for thromboembolism, bridging therapy with LMWH or UFH is recommended (bridging means stopping the warfarin and using anticoagulant doses of the LMWH or UFH for a short period to prevent clotting).
Discontinue therapeutic-dose SC LMWH 24 hours before surgery (stop the UFH IV therapy 4 - 6 hours before surgery).
Patients at low risk for thromboembolism do not require bridging; stop the warfarin and restart after surgery when hemostasis is achieved.

■ If INR is still elevated 1- 2 days before surgery, give low- dose vitamin K (1- 2 mg).

■ If reversal of warfarin is needed in a patient requiring an urgent surgical procedure, give low-dose (2.5- 5mg) IV or oral vitamin K.

■ Resume warfarin therapy 12- 24 hours after the surgery, when there is adequate hemostasis.

Answer 122

A

Symptoms of a DVT include pain in the affected limb and unilateral lower extremity swelling.
DVTs can be diagnosed with an ultrasound (or MRI or venography, in some cases).
A D-dimer (a lab test) can aid in the diagnosis.
If a PE is suspected, it is diagnosed with a pulmonary CT angiogram.

Answer 123

A

The CHEST guidelines provide specific recommendations for the prevention of VTE depending on the patient’s level of risk.
UFH, LMWHs, fondaparinux, rivaroxaban, apixaban and dabigatran are all approved for VTE prophylaxis.
If patients have a contraindication to anticoagulants (such as an active bleed) or have a high risk for bleeding, they will need non- drug alternatives to prevent VTE.
These options include intermittent pneumatic compression (IPC) devices or graduated compression stockings.
For long-distance travelers at risk for VTE (previous VTE, recent surgery or trauma, active malignancy, pregnancy, estrogen use, advanced age, limited mobility, severe obesity or known thrombophilic disorder), the following recommendations will dec VTE risk:
– frequent ambulation, calf muscle exercises, sitting in an aisle seat and using graduated compression stockings with 15- 30 mmHg of pressure at the ankle during travel.
– Aspirin or anticoagulants should not be used.

Answer 124

A

Surgery
Major trauma or lower extremity injury
Immobility
Cancer or chemotherapy
Previous VTE
Pregnancy and postpartum period
Estrogen-containing medications or SERMs
Erythropoiesis-stimulating agents
Increasing age
Obesity
Inherited or acquired thrombophilia (antithrombin deficiency, factor V Leiden, antiphospholipid syndrome, protein C or protein S deficiency)
Acute medical illness
Venous compression (tumor, hematoma, arterial abnormality)
Inflammatory bowel disease
Nephrotic syndrome
Myeloproliferative disorders
Paroxysmal nocturnal hemoglobinuria
Central venous catheterization

Answer 125

A

Any VTE that is caused by surgery or a reversible risk factor should be treated for 3 months.
If the VTE is unprovoked (unknown cause), extending therapy longer than three months is recommended, as long as the patient’s bleeding risk
is low-to-moderate.
If the risk of bleeding is high, limit the treatment to three months.
If a patient has two unprovoked VTE episodes, long-term treatment can be considered.
Estrogen-containing medications and selective estrogen receptor modulators (SERMs) are contraindicated in patients with history of, or current, VTE and should be discontinued.
For patients without cancer, dabigatran and the oral factor Xa inhibitors (rivaroxaban, apixaban and edoxaban) are preferred over warfarin for the first three months of treatment for a DVT in the leg or a PE.
For patients with cancer, LMWH is preferred over all oral anticoagulants (including warfarin).
In patients with an unprovoked DVT or PE who are stopping anticoagulation, aspirin is recommended to prevent recurrence (if there are no CI).

Answer 126

A

AFib/ Aflutter –> Heart clots Risk –> Can go to brain and cause a stroke (cardioembolic stroke) or transient ischemic attack (TIA).
– !! Stroke prevention !!
AFib and Aflutter are common in patients with heart valve problems.
– Some require valve replacement surgery.
Mechanical (prosthetic) Valve
Animal (sometimes called a bioprosthetic) valve
Patients with mechanical heart valves have the highest risk for clotting/strokes and are treated with warfarin only.
– Factor Xa inhibitors and DTI are not approved for this population.
The majority of patients with AFib/AFlutter do not have heart valve involvement (called nonvalvular AFib), but they still require evaluation of their stroke risk.
The CHEST guidelines use the CHADS-VASc scoring system to estimate risk of stroke in AFib/AFlutter and guide therapy.

Answer 127

A

AFib > 48 hours or unknown duration:
– Anticoagulation (if warfarin, target INR 2-3) for at least 3 weeks prior to and
– 4 weeks after cardioversion (regardless of method - electrical or pharmacologic) when normal sinus rhythm is restored.
AFib <= 48 hours duration undergoing elective cardioversion:
– Start full therapeutic anticoagulation at presentation
– Perform cardioversion, and
– Continue full anticoagulation for at least 4 weeks while patient is in normal sinus rhythm.
For patients staying in AFib,
– Chronic anticoagulation therapy may be needed for stroke prevention.
– Treatment depends on the number of risk factors present.

Answer 128

A

Count the number of risk factors the patient has, then select the recommended therapy.
The higher the score, the greater the stroke risk and the more intensive the anticoagulant recommendations.
– CHF: 1
– HTN: 1
– Age >= 75 Years: 2
– Diabetes: 1
– Stroke/TIA Hx: 2
– Vascular Disease: 1 (prior Ml, PAD, aortic plaque)
– Age 65-74 Years: 1
– Sex: Female: 1

Recommendations:

No anticoagulation recommended:
– Score = 0 (males)
– Score = 1 (females)
Oral anticoagulation may be considered.
– Score >= 1(males)
– Score >= 2 (females)
Oral anticoagulation is recommended.
Non-vitamin K oral anticoagulant (DOAC) is recommended over warfarin.
– Score >= 2 {males)
– Score >= 3 (females)

DOAC:apixaban,rivaroxaban,edoxaban,dabigatran

Answer 129

A

For prevention and treatment of VTE in pregnant women, LMWH is preferred over UFH.
Pneumatic compression devices can be used alone or with LMWH in select patients.
Since warfarin is teratogenic, women who require chronic warfarin therapy for mechanical heart valves or inherited thrombophilias are generally converted to LMWH during pregnancy.
– They may be switched back to warfarin after the 13th week of pregnancy, then back to LMWH close to delivery.
When LMWH is used in pregnancy, anti-Xa levels are recommended to monitor therapy.
The oral factor Xa inhibitors and direct thrombin inhibitors have not been adequately studied in pregnancy and are not recommended .

Answer 130

A

■ Can cause serious and life-threatening bleeding/bruising.
■ Tell physicians and dentists that you are using this medication before any surgery is performed.
■ Call your healthcare provider right away if you fall or injure yourself, especially if you hit your head.
■ Avoid alcohol.
■ Many drug interactions.
■ Missed dose: take as soon as possible on the same day. Do not take a double dose the next day to make up for a missed dose.

Answer 131

A

■ Take with a full glass of water; swallow capsules whole.
■ Can cause dyspepsia.
■ Only open one bottle of dabigatran at a time. After opening a bottle of dabigatran, use within 4 months.
■ Keep dabigatran in the original bottle or blister package. Do not put dabigatran in pill boxes or pill organizers.
■ Missed dose: if your next dose is less than six hours away, skip the missed dose.

Answer 132

A

■ Atrial fibrillation: take once daily with the evening meal.
■ Blood clots in the veins of your legs or in the lungs: take once or twice daily as prescribed with food at the same time each day.
■ Missed dose: if taken twice daily, can take two doses at the same time to make up for the missed dose.

Answer 133

A

■ SQ: choose an area on the right or left side of your abdomen, at least two inches from the belly button.
Wash your hands and clean the site.

■ Remove the needle cap by pulling it straight off the syringe.
Do not twist the cap off as this can bend the needle.

■ Do not expel the air bubble in the syringe prior to injection unless your healthcare provider has advised you to do so.

■ Hold the syringe like a pencil. Pinch an inch of skin to make a fold. Insert the full length of the needle straight down at a 90 degree angle into the fold of the skin.

■ Press the plunger with your thumb until the syringe is empty.

■ Pull the needle straight out at the same angle that it was inserted, and release the skin fold.

■ Point the needle down and away from yourself and others, and push down on the plunger to activate the safety shield.

■ Do not rub the site of injection as this can lead to bruising. Place the used syringe in the sharps collector.

Answer 134

A

■ Take at the same time every day.
■ Ask your pharmacist if your tablet looks different.
■ Can rarely cause:
o Purple toe syndrome (painful toes and purple discoloration).
o Death of skin tissue (with pain).
■ Frequent blood monitoring required (INR).
■ Consistent intake of vitamin K required (mainly found in green, leafy vegetables).

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Chapter 34 - Anticoagulation Flashcards

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