Contraindicated in:
Use Cautiously in:
GI: ↑amylase, ↑ liver enzymes, ACUTE EXACERBATION OF HBV, diarrhea, LACTIC ACIDOSIS/HEPATOMEGALY WITH STEATOSIS, nausea.
GU: ACUTE RENAL FAILURE/FANCONI SYNDROME.
Hemat: neutropenia.
Metab: hyperlipidemia.
MS: ↑creatine kinase.
Neuro: abnormal dreams, dizziness, fatigue, headache, insomnia.
Misc: immune reconstitution syndrome.
Drug-Drug:
Drug-Natural Products:
Renal Impairment
Therapeutic Classification: antiretrovirals
Pharmacologic Classification: nucleoside reverse transcriptase inhibitors, integrase strand transfer inhibitors (INSTI)
Bictegravir
Absorption: Extent of absorption following oral administration unknown.
Distribution: Unknown.
Protein Binding: >99%.
Metabolism/Excretion: Primarily metabolized by the CYP3A4 isoenzyme and UGT1A1 in the liver; 60% excreted in feces, 35% excreted in urine.
Half-life: 17.3 hr;.
Emtricitabine
Absorption: Well absorbed (93%) following oral administration.
Distribution: Unknown.
Metabolism/Excretion: Undergoes some metabolism, 70% excreted in urine, 14% excreted in feces.
Half-life: 10.4 hr.
Tenofovir Alafenamide
Absorption: Tenofovir alafenamide is a prodrug, which is hydrolyzed into tenofovir, the active component; absorption enhanced by high-fat meals.
Distribution: Unknown.
Metabolism/Excretion: Tenofovir is phosphorylated to tenofovir diphosphate (active metabolite); 32% excreted in feces, <1% excreted in urine.
Half-life: Tenofovir alafenamide: 0.51 hr; Tenofovir diphosphate: 150180 hr.
(plasma concentrations)
ROUTE | ONSET | PEAK | DURATION |
---|---|---|---|
bictegravir PO | unknown | 24 hr | 24 hr |
emtricitabine PO | unknown | 1.52 hr | 24 hr |
tenofovir PO | unknown | 0.52 hr | 24 hr |