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Pronunciation

da-ROO-na-veer/koe-BIK-i-stat/

Classifications

Therapeutic Classification: antiretrovirals, pharmacoenhancers

Pharmacologic Classification: protease inhibitors, enzyme inhibitors

Indications

REMS

Action

  • Darunavir: Inhibits HIV-1 protease, selectively inhibiting the cleavage of HIV-encoded specific polyproteins in infected cells. This prevents the formation of mature virus particles.
  • Cobicistat: Strongly inhibits CYP3A enzymes, enhancing systemic exposure to darunavir.
Therapeutic effects:
  • Increased CD4 cell counts and decreased viral load with subsequent slowed progression of HIV infection and its sequelae.

Pharmacokinetics

Darunavir

Absorption: Food enhances oral absorption.

Distribution: Unknown.

Protein Binding: 95% bound to plasma proteins.

Metabolism/Excretion: Extensively metabolized by CYP3A enzyme system. 41% eliminated unchanged in feces, 8% in urine.

Half-Life: 15 hr.

Cobicistat

Absorption: Absorption follows oral administration.

Distribution: Unknown.

Protein Binding: 97–98%.

Metabolism/Excretion: Metabolized by CYP3A and to a small extent by CYP2D6; 86.2 eliminated in feces, 8.2% in urine.

Half-Life: 3–4 hr.

Time/Action Profile

ROUTEONSETPEAKDURATION
darunavirunknown2.5–4 hr12 hr
cobicistatunknown3 hr24 hr



Contraind./Precautions

Contraindicated in:

Use Cautiously in:

Adv. Reactions/Side Effects

Derm: rash, STEVENS-JOHNSON SYNDROME

Endo: Graves' disease, hyperglycemia

GI: abdominal pain, autoimmune hepatitis, diarrhea, HEPATOTOXICITY, nausea, vomiting

MS: polymyositis

Neuro: Guillain-Barré syndrome, headache

Misc: immune reconstitution syndrome, redistribution of body fat

Interactions

Drug-drug:

Drug-Natural Products:

Route/Dosage

Availability

Assessment

Lab Test Considerations:

Implementation

Patient/Family Teaching

Evaluation/Desired Outcomes

US Brand Names

Prezcobix