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{{NOAC}}
{{A Scientific Statement From the American Heart Association - 2017}}
{{CMG}},{{AE}}{{AKK}}
{{CMG}},{{AE}}{{AKK}}


==Management of Patients on Non–Vitamin K Antagonist Oral Anticoagulants (NOACs) in the Acute Care and Periprocedural Setting==
==Management of Patients on Non–Vitamin K Antagonist Oral Anticoagulants (NOACs) in the Acute Care and Periprocedural Setting==
===A Scientific Statement From the American Heart Association - 2017===


===Comparison Among NOACs===
===Comparison Among NOACs===


{| class="wikitable" style="width: 80%; text-align: justify;"  
{| class="wikitable" style="width: 90%; text-align: justify;"  


! style="width:20%" |   
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| '''Volume of distribution''' || 50–70 L || 50 L || 21 L || 107 L
| '''Volume of distribution''' || 50–70 L || 50 L || 21 L || 107 L
|-  
|-  
| '''Plasma t1/2''' || 12–17 h; Elderly 14–17 h; Mild to moderate renal impairment 15–18 h; Severe renal impairment 28 h|| 5–9 h; Elderly 11–13 h || ~12 h (8–15 h) || 10–14 h
| '''Plasma ''' || 12–17 h;  
Elderly 14–17 h;  
 
Mild to moderate renal impairment 15–18 h;
 
Severe renal impairment   28 h
| 5–9 h;
Elderly 11–13 h  
| ~12 h (8–15 h) || 10–14 h
|-  
|-  
| '''Metabolism''' || Hepatic and plasma hydrolysis to active dabigatran; Hepatic glucuronidation to active metabolites (<10%); P-gp substrate || Hepatic: oxidation by CYP3A4/5, CYP2J2; hydrolysis to inactive metabolites (51%); P-gp substrate; No major or active circulating metabolites; Substrate of P-gp and ABCG2 (BCRP) || Hepatic: 25% mainly by CYP3A4/5; lesser by CYP1A2, CYP2C8, CYP2C9, CYP2C19, CYP2J2; O-demethylation and hydroxylation; No active circulating metabolites; Substrate of CYP3A4, P-gp, BCRP || Minimal CYP3A4 hydrolysis, conjugation, oxidation; Active metabolite (M-4, <10% of parent); P-gp substrate
| '''Metabolism''' || Hepatic and plasma hydrolysis to active dabigatran;
Hepatic glucuronidation to active metabolites (<10%); P-gp substrate  
| Hepatic: oxidation by CYP3A4/5, CYP2J2; hydrolysis to inactive metabolites (51%); P-gp substrate;
No major or active circulating metabolites; Substrate of P-gp and ABCG2 (BCRP)  
| Hepatic: 25% mainly by CYP3A4/5; lesser by CYP1A2, CYP2C8, CYP2C9, CYP2C19, CYP2J2;
O-demethylation and hydroxylation; No active circulating metabolites; Substrate of CYP3A4, P-gp, BCRP  
| Minimal CYP3A4 hydrolysis, conjugation, oxidation; Active metabolite (M-4, <10% of parent); P-gp substrate
|-  
|-  
| '''Excretion''' || Renal (~80%) after IV administration; After oral, 7% recovered in urine, 86% in feces || Feces (28%): 7% active, 21% inactive metabolites || Biliary and direct intestinal excretion || Metabolism and biliary/ intestinal excretion accounts for the rest
| '''Excretion''' || Renal (~80%) after IV administration;
After oral, 7% recovered in urine, 86% in feces  
| Feces (28%): 7% active, 21% inactive metabolites || Biliary and direct intestinal excretion || Metabolism and biliary/ intestinal excretion accounts for the rest
|-  
|-  
| colspan="5" | '''Dosing'''  
| colspan="5" | '''Dosing'''  
|-  
|-  
| '''Nonvalvular AF''' || CrCl >30 mL/min: 150 mg BID; CrCl 15–30 mL/min:   
| '''Nonvalvular AF''' || CrCl >30 mL/min: 150 mg BID; CrCl 15–30 mL/min:   
75 mg BID; CrCl <15 mL/min or on dialysis: Not recommended; CrCl 30–50 mL/min with concomitant P-gp inhibitors: 75 mg BID;   CrCl <30 mL/min with concomitant P-gp inhibitors: Avoid coadministration  
75 mg BID; CrCl <15 mL/min or on dialysis: Not recommended;
| CrCl >50 mL/min: 20 mg daily with evening meal; CrCl 15–50 mL/min: 15 mg daily with evening meal; Not recommended for CrCl <15 mL/min or on dialysis in patients with AF || 5 mg BID; 2.5 mg BID, if 2 of 3 characteristics: Cr ≥1.5 mg/dL, age ≥80 y, weight ≤60 kg || CrCl >50 to ≤95 mL/min: 60 mg daily; CrCl 15–50 mL/min: 30 mg daily; NOT recommended for CrCl >95 mL/min
 
CrCl 30–50 mL/min with concomitant P-gp inhibitors: 75 mg BID;    
 
CrCl <30 mL/min with concomitant P-gp inhibitors: Avoid coadministration  
| CrCl >50 mL/min: 20 mg daily with evening meal; CrCl 15–50 mL/min: 15 mg daily with evening meal;
Not recommended for CrCl <15 mL/min or on dialysis in patients with AF  
| 5 mg BID;
2.5 mg BID, if 2 of 3 characteristics: Cr ≥1.5 mg/dL, age ≥80 y, weight ≤60 kg  
| CrCl >50 to ≤95 mL/min: 60 mg daily; CrCl 15–50 mL/min: 30 mg daily;  
NOT recommended for CrCl >95 mL/min
|-  
|-  
| '''DVT or PE treatment''' || CrCl >30 mL/min: 150 mg BID after 5-10 d parenteral anticoagulation; CrCl ≤30 mL/min or on dialysis: Not recommended || 15 mg BID with food  rst 21 d for initial treatment, then 20 mg once daily with food; Not recommended for CrCl <30 mL/min in patients with DVT or PE || 10 mg BID x 7 d, then 5 mg BID || 60 mg once daily; CrCl 15–50 mL/min or weight ≤60 kg or on certain P-gp inhibitors: 30 mg once daily
| '''DVT or PE treatment''' || CrCl >30 mL/min: 150 mg BID after 5-10 d parenteral anticoagulation;
CrCl ≤30 mL/min or on dialysis: Not recommended  
| 15 mg BID with food  rst 21 d for initial treatment, then 20 mg once daily with food; Not recommended for CrCl <30 mL/min in patients with DVT or PE || 10 mg BID x 7 d, then 5 mg BID || 60 mg once daily; CrCl 15–50 mL/min or weight ≤60 kg or on certain P-gp inhibitors: 30 mg once daily
|-  
|-  
| '''↓ in recurrent DVT/PE''' || CrCl >30 mL/min: 150 mg BID after 5–10 d parenteral anticoagulation; CrCl ≤30 mL/min or on dialysis: Not recommended || 20 mg daily with food || 2.5 mg BID ||  
| '''↓ in recurrent DVT/PE''' || CrCl >30 mL/min: 150 mg BID after 5–10 d parenteral anticoagulation;
CrCl ≤30 mL/min or on dialysis: Not recommended  
| 20 mg daily with food || 2.5 mg BID ||  
|-  
|-  
| '''DVT,PE prophylaxis after hip or knee replacement''' || After hip replacement surgery: CrCl >30 mL/min after achievement of hemostasis: If given day of surgery, 110 mg 1–4 h postop; after day of surgery 220 mg once daily x 28–35 d CrCl ≤30 mL/min or on dialysis: Not recommended CrCl <50 mL/min with concomitant P-gp inhibitors: Avoid coadministration || Initial dose 6–10 h after surgery provided homeostasis established; 10 mg daily with or without food x 35 d for hip replacement, x 12 d for knee replacement || 2.5 mg BIDx35 d after hip replacement surgery or x 12 d after knee replacement surgery ||  
| '''DVT, PE prophylaxis after hip or knee replacement''' || After hip replacement surgery: CrCl >30 mL/min after achievement of hemostasis: If given day of surgery, 110 mg 1–4 h postop;
after day of surgery 220 mg once daily x 28–35 d CrCl ≤30 mL/min or on dialysis: Not recommended CrCl <50 mL/min with concomitant   P-gp inhibitors: Avoid coadministration  
| Initial dose 6–10 h after surgery provided homeostasis established; 10 mg daily with or without food x 35 d for hip replacement, x 12 d for knee replacement || 2.5 mg BIDx35 d after hip replacement surgery or x 12 d after knee replacement surgery ||  
|-  
|-  
| '''Additional dosing comments''' || || Avoid use with patients with moderate-severe hepatic impairment (Child- Pugh class B/C) or hepatic disease with coagulopathy; 15-20 mg taken with food; 10 mg with or without food || Not recommended in patients with severe hepatic impairment (Child-Pugh class C) || Not recommended with CrCl <15 mL/min; Not recommended
| '''Additional                 dosing comments''' || || Avoid use with patients with moderate-severe hepatic impairment (Child- Pugh class B/C) or hepatic disease with coagulopathy; 15-20 mg taken with food; 10 mg with or without food || Not recommended in patients with severe hepatic impairment (Child-Pugh class C) || Not recommended with CrCl <15 mL/min;                     Not recommended
in patients with moderate-severe hepatic impairment (Child-Pugh class B/C)
in patients with moderate-severe hepatic impairment (Child-Pugh class B/C)
|-  
|-  
| '''Therapeutic measurement''' || Routine not required, To detect presence: aPTT, ECT (if available), TT; aPTT >2.5 times control may indicate over anticoagulation; Renal function, CBC periodically, at least annually || Routine not required; To detect presence: PT, aPTT, antifactor Xa activity; Renal function, CBC periodically, at least annually; hepatic function || Routine not required; To detect presence: PT, aPTT, antifactor Xa activity; Renal function, CBC periodically, at least annually || Routine not required; Prolongs PT, aPTT, antifactor Xa activity; Renal function, CBC periodically, at least annually
| '''Therapeutic measurement''' || Routine not required, To detect presence: aPTT, ECT (if available), TT;           aPTT >2.5 times control may indicate over anticoagulation;             Renal function, CBC periodically, at least annually || Routine not required; To detect presence: PT, aPTT, antifactor Xa activity;   Renal function, CBC periodically, at least annually;    
Hepatic function  
| Routine not required; To detect presence: PT, aPTT, antifactor Xa activity;  
Renal function, CBC periodically, at least annually  
| Routine not required; Prolongs PT, aPTT, antifactor Xa activity;  
Renal function, CBC periodically, at least annually
|-  
|-  
| colspan="5" | '''AC''' indicates anticoagulant; '''AF''', atrial  brillation; '''aPTT,''' activated partial thromboplastin time; '''BID''', twice daily; '''CBC''', complete blood count; CrCl, creatinine clearance; '''DVT''', deep vein thrombosis; '''ECT,''' ecarin clotting time; IV, intravenous; '''NOACs''', non–vitamin K antagonist oral anticoagulants; '''PE''', pulmonary embolism; P-gp, P-glycoprotein; '''PT''', prothrombin time; and '''TT''', thrombin time.  
| colspan="5" | '''AC''' indicates anticoagulant; '''AF''', atrial  brillation; '''aPTT,''' activated partial thromboplastin time; '''BID''', twice daily; '''CBC''', complete blood count; CrCl, creatinine clearance; '''DVT''', deep vein thrombosis; '''ECT,''' ecarin clotting time; IV, intravenous; '''NOACs''', non–vitamin K antagonist oral anticoagulants; '''PE''', pulmonary embolism; P-gp, P-glycoprotein; '''PT''', prothrombin time; and '''TT''', thrombin time.  
|}
===NOAC Drug Interactions===
{| class="wikitable" style="width: 90%; text-align: justify;"
! style="width:15%" | '''NOAC'''
! style="width:30%" | '''Interacting Medications'''
! style="width:25%" | '''Effect on NOAC'''
! style="width:30%" | '''Labeled Guidance; Comments'''
|-
| bgcolor="LightBlue" rowspan="3" | '''Dabigatran''' || P-gp inducer: rifampin || ↓ Dabigatran exposure || Concomitant use should generally be avoided.
|-
| P-gp inhibitors: ketoconazole, dronedarone || ↑ Dabigatran exposure if concomitant moderate renal impairment || If moderate renal impairment (CrCl 30–50 mL/min) ↓ to 75 mg BID during concomitant use
|-
| P-gp inhibitors: ketoconazole, dronedarone, verapamil, amiodarone, quinidine, clarithromycin, ticagrelor || ↑ Dabigatran exposure if concomitant severe renal impairment ||If severe renal impairment (CrCl 15–30 mL/ min) avoid concomitant use
|-
| bgcolor="LightBlue" rowspan="2" | '''Apixaban''' || Strong dual P-gp and CYP3A4 inducers: rifampin, carbamazepine, phenytoin, St. John’s wort || ↓ Apixaban exposure || Avoid concomitant use
|-
| Strong dual P-gp and CYP3A4 inhibitors: ketoconazole, itraconazole, ritonavir, clarithromycin || ↑ Apixaban exposure || In patients on 5 mg or 10 mg BID, ↓ dose by 50% when coadministered; Avoid coadministration on 2.5 mg BID
|-
|  bgcolor="LightBlue" rowspan="3" | '''Rivaroxaban''' || Combined P-gp and strong CYP3A4 inducers: rifampin, carbamazepine, phenytoin, St. John’s wort || ↓ Rivaroxaban exposure || Avoid concomitant use; may decrease rivaroxaban efficacy
|-
| Combined P-gp and strong CYP3A4 inhibitors: ketoconazole, itraconazole, HIV protease inhibitors (ritonavir, lopinavir/ ritonavir, indinavir), conivaptan || ↓ Rivaroxaban exposure || Avoid concomitant use
|-
| Combined P-gp and moderate CYP3A4 inhibitors: diltiazem, verapamil, amiodarone, dronedarone, erythromycin || ↑ Rivaroxaban exposure in patients with renal impairment || '''-''' In patients with CrCl 15 to <80 mL/min, rivaroxaban should not be used concomitantly unless the potential benefit justifies the potential risks
'''-''' No evidence of interaction observed in ROCKET AF between treatment assignment and outcomes in patients using ≥1 combined P-gp and moderate 3A4 inhibitors (including amiodarone, diltiazem, and verapamil)
|-
| bgcolor="LightBlue" rowspan="3" | '''Edoxaban''' || P-gp inducer: rifampin || ↓ Edoxaban exposure || Avoid concomitant use
|-
| Strong P-gp inhibitors: ritonavir, nelfinavir, saquinavir, indinavir, cyclosporine || ↑ Edoxaban exposure || Avoid concomitant use in patients taking edoxaban for treatment of VTE
|-
| P-gp inhibitors: verapamil, quinidine, azithromycin, clarithromycin, itraconazole, ketoconazole || ↑ Edoxaban exposure || '''-''' ↓ to 30 mg daily during concomitant administration for patients taking edoxaban for the treatment of VTE
'''-''' Dose reduction is not recommended  for  AF  indications                 
'''-''' In ENGAGE AF, a ↓ dose of edoxaban as a result of concomitant P-gp inhibitor use (verapamil, quinidine, dronedarone) was associated with ↓ edoxaban exposure and a relative ↑ in risk of stroke or systemic embolism with edoxaban relative to warfarin
|-
| colspan="4" | '''AF''', atrial fibrillation; '''BID''', twice daily; '''CrCl,''' creatinine clearance; '''ENGAGE AF''', Effective Anticoagulation With Factor Xa Next Generation in Atrial Fibrillation trial; '''NOAC''', non–vitamin K antagonist oral anticoagulant; '''P-gp''', P-glycoprotein; '''ROCKET AF''', Rivaroxaban Once Daily Oral Direct Factor Xa Inhibition Compared with Vitamin K Antagonism for Prevention of Stroke and Embolism Trial in Atrial Fibrillation; and '''VTE''', venous thromboembolism.
|}
|}

Latest revision as of 01:25, 1 November 2017

Template:NOAC Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1],Associate Editor(s)-in-Chief: Arzu Kalayci, M.D. [2]

Management of Patients on Non–Vitamin K Antagonist Oral Anticoagulants (NOACs) in the Acute Care and Periprocedural Setting

A Scientific Statement From the American Heart Association - 2017

Comparison Among NOACs

Dabigatran Rivaroxaban Apixaban Edoxaban
Approved indications Nonvalular AF ↓ Risk of stroke and systemic embolism Nonvalular AF ↓ Risk of stroke and systemic embolism Nonvalular AF ↓ Risk of stroke and systemic embolism Nonvalular AF ↓ Risk of stroke and systemic embolism. Limitation: should not use in patients with CrCl >95 mL/min as a result of ↑ risk of ischemic stroke compared with warfarin at 60 mg
DVT,PE Treatment after 5–10 d parenteral AC ↓ Recurrence Prophylaxis after hip replacement DVT,PE Treatment ↓ Recurrence Prophylaxis after hip or knee replacement DVT,PE Treatment ↓ Recurrence Prophylaxis after hip replacement DVT,PE ↓ Recurrence Treatment after 5–10 d initial parenteral AC
Mechanism of action Direct thrombin inhibitor Factor Xa inhibitor Factor Xa inhibitor Factor Xa inhibitor
Time to peak 1 h; delayed to 2 h with food 2–4 h 3–4 h 1–2 h
Bioavailability 3%–7% 10-mg dose: 80%–100% ; 20-mg dose: 66% ; ↑ With food ~50% 62%
Plasma protein binding 35% 92%–95% ~87% 55%
Volume of distribution 50–70 L 50 L 21 L 107 L
Plasma t½ 12–17 h;

Elderly 14–17 h;

Mild to moderate renal impairment 15–18 h;

Severe renal impairment 28 h

5–9 h;

Elderly 11–13 h

~12 h (8–15 h) 10–14 h
Metabolism Hepatic and plasma hydrolysis to active dabigatran;

Hepatic glucuronidation to active metabolites (<10%); P-gp substrate

Hepatic: oxidation by CYP3A4/5, CYP2J2; hydrolysis to inactive metabolites (51%); P-gp substrate;

No major or active circulating metabolites; Substrate of P-gp and ABCG2 (BCRP)

Hepatic: 25% mainly by CYP3A4/5; lesser by CYP1A2, CYP2C8, CYP2C9, CYP2C19, CYP2J2;

O-demethylation and hydroxylation; No active circulating metabolites; Substrate of CYP3A4, P-gp, BCRP

Minimal CYP3A4 hydrolysis, conjugation, oxidation; Active metabolite (M-4, <10% of parent); P-gp substrate
Excretion Renal (~80%) after IV administration;

After oral, 7% recovered in urine, 86% in feces

Feces (28%): 7% active, 21% inactive metabolites Biliary and direct intestinal excretion Metabolism and biliary/ intestinal excretion accounts for the rest
Dosing
Nonvalvular AF CrCl >30 mL/min: 150 mg BID; CrCl 15–30 mL/min:

75 mg BID; CrCl <15 mL/min or on dialysis: Not recommended;

CrCl 30–50 mL/min with concomitant P-gp inhibitors: 75 mg BID;

CrCl <30 mL/min with concomitant P-gp inhibitors: Avoid coadministration

CrCl >50 mL/min: 20 mg daily with evening meal; CrCl 15–50 mL/min: 15 mg daily with evening meal;

Not recommended for CrCl <15 mL/min or on dialysis in patients with AF

5 mg BID;

2.5 mg BID, if 2 of 3 characteristics: Cr ≥1.5 mg/dL, age ≥80 y, weight ≤60 kg

CrCl >50 to ≤95 mL/min: 60 mg daily; CrCl 15–50 mL/min: 30 mg daily;

NOT recommended for CrCl >95 mL/min

DVT or PE treatment CrCl >30 mL/min: 150 mg BID after 5-10 d parenteral anticoagulation;

CrCl ≤30 mL/min or on dialysis: Not recommended

15 mg BID with food rst 21 d for initial treatment, then 20 mg once daily with food; Not recommended for CrCl <30 mL/min in patients with DVT or PE 10 mg BID x 7 d, then 5 mg BID 60 mg once daily; CrCl 15–50 mL/min or weight ≤60 kg or on certain P-gp inhibitors: 30 mg once daily
↓ in recurrent DVT/PE CrCl >30 mL/min: 150 mg BID after 5–10 d parenteral anticoagulation;

CrCl ≤30 mL/min or on dialysis: Not recommended

20 mg daily with food 2.5 mg BID
DVT, PE prophylaxis after hip or knee replacement After hip replacement surgery: CrCl >30 mL/min after achievement of hemostasis: If given day of surgery, 110 mg 1–4 h postop;

after day of surgery 220 mg once daily x 28–35 d CrCl ≤30 mL/min or on dialysis: Not recommended CrCl <50 mL/min with concomitant P-gp inhibitors: Avoid coadministration

Initial dose 6–10 h after surgery provided homeostasis established; 10 mg daily with or without food x 35 d for hip replacement, x 12 d for knee replacement 2.5 mg BIDx35 d after hip replacement surgery or x 12 d after knee replacement surgery
Additional dosing comments Avoid use with patients with moderate-severe hepatic impairment (Child- Pugh class B/C) or hepatic disease with coagulopathy; 15-20 mg taken with food; 10 mg with or without food Not recommended in patients with severe hepatic impairment (Child-Pugh class C) Not recommended with CrCl <15 mL/min; Not recommended

in patients with moderate-severe hepatic impairment (Child-Pugh class B/C)

Therapeutic measurement Routine not required, To detect presence: aPTT, ECT (if available), TT; aPTT >2.5 times control may indicate over anticoagulation; Renal function, CBC periodically, at least annually Routine not required; To detect presence: PT, aPTT, antifactor Xa activity; Renal function, CBC periodically, at least annually;

Hepatic function

Routine not required; To detect presence: PT, aPTT, antifactor Xa activity;

Renal function, CBC periodically, at least annually

Routine not required; Prolongs PT, aPTT, antifactor Xa activity;

Renal function, CBC periodically, at least annually

AC indicates anticoagulant; AF, atrial brillation; aPTT, activated partial thromboplastin time; BID, twice daily; CBC, complete blood count; CrCl, creatinine clearance; DVT, deep vein thrombosis; ECT, ecarin clotting time; IV, intravenous; NOACs, non–vitamin K antagonist oral anticoagulants; PE, pulmonary embolism; P-gp, P-glycoprotein; PT, prothrombin time; and TT, thrombin time.

NOAC Drug Interactions

NOAC Interacting Medications Effect on NOAC Labeled Guidance; Comments
Dabigatran P-gp inducer: rifampin ↓ Dabigatran exposure Concomitant use should generally be avoided.
P-gp inhibitors: ketoconazole, dronedarone ↑ Dabigatran exposure if concomitant moderate renal impairment If moderate renal impairment (CrCl 30–50 mL/min) ↓ to 75 mg BID during concomitant use
P-gp inhibitors: ketoconazole, dronedarone, verapamil, amiodarone, quinidine, clarithromycin, ticagrelor ↑ Dabigatran exposure if concomitant severe renal impairment If severe renal impairment (CrCl 15–30 mL/ min) avoid concomitant use
Apixaban Strong dual P-gp and CYP3A4 inducers: rifampin, carbamazepine, phenytoin, St. John’s wort ↓ Apixaban exposure Avoid concomitant use
Strong dual P-gp and CYP3A4 inhibitors: ketoconazole, itraconazole, ritonavir, clarithromycin ↑ Apixaban exposure In patients on 5 mg or 10 mg BID, ↓ dose by 50% when coadministered; Avoid coadministration on 2.5 mg BID
Rivaroxaban Combined P-gp and strong CYP3A4 inducers: rifampin, carbamazepine, phenytoin, St. John’s wort ↓ Rivaroxaban exposure Avoid concomitant use; may decrease rivaroxaban efficacy
Combined P-gp and strong CYP3A4 inhibitors: ketoconazole, itraconazole, HIV protease inhibitors (ritonavir, lopinavir/ ritonavir, indinavir), conivaptan ↓ Rivaroxaban exposure Avoid concomitant use
Combined P-gp and moderate CYP3A4 inhibitors: diltiazem, verapamil, amiodarone, dronedarone, erythromycin ↑ Rivaroxaban exposure in patients with renal impairment - In patients with CrCl 15 to <80 mL/min, rivaroxaban should not be used concomitantly unless the potential benefit justifies the potential risks

- No evidence of interaction observed in ROCKET AF between treatment assignment and outcomes in patients using ≥1 combined P-gp and moderate 3A4 inhibitors (including amiodarone, diltiazem, and verapamil)

Edoxaban P-gp inducer: rifampin ↓ Edoxaban exposure Avoid concomitant use
Strong P-gp inhibitors: ritonavir, nelfinavir, saquinavir, indinavir, cyclosporine ↑ Edoxaban exposure Avoid concomitant use in patients taking edoxaban for treatment of VTE
P-gp inhibitors: verapamil, quinidine, azithromycin, clarithromycin, itraconazole, ketoconazole ↑ Edoxaban exposure - ↓ to 30 mg daily during concomitant administration for patients taking edoxaban for the treatment of VTE

- Dose reduction is not recommended for AF indications

- In ENGAGE AF, a ↓ dose of edoxaban as a result of concomitant P-gp inhibitor use (verapamil, quinidine, dronedarone) was associated with ↓ edoxaban exposure and a relative ↑ in risk of stroke or systemic embolism with edoxaban relative to warfarin

AF, atrial fibrillation; BID, twice daily; CrCl, creatinine clearance; ENGAGE AF, Effective Anticoagulation With Factor Xa Next Generation in Atrial Fibrillation trial; NOAC, non–vitamin K antagonist oral anticoagulant; P-gp, P-glycoprotein; ROCKET AF, Rivaroxaban Once Daily Oral Direct Factor Xa Inhibition Compared with Vitamin K Antagonism for Prevention of Stroke and Embolism Trial in Atrial Fibrillation; and VTE, venous thromboembolism.
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