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Literature DB >> 9486958

HIV protease inhibitors, saquinavir, indinavir and ritonavir: inhibition of CYP3A4-mediated metabolism of testosterone and benzoxazinorifamycin, KRM-1648, in human liver microsomes.

T Inaba¹, N E Fischer, D S Riddick, D J Stewart, T Hidaka.

Abstract

The protease inhibitors, ritonavir, indinavir and saquinavir, the most potent anti-HIV drugs developed to date, interact with many drugs by competing for CYP3A4, an enzyme central to the metabolism of a wide variety of compounds. Human liver microsomes were used to compare inhibition by these three protease inhibitors. The inhibition was the greatest with ritonavir and indinavir and less potent with saquinavir.

Entities: Chemical Gene Species

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Year: 1997 PMID： 9486958 DOI： 10.1016/s0378-4274(97)00098-2

Source DB: PubMed Journal: Toxicol Lett ISSN： 0378-4274 Impact factor: 4.372

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Cited

8 in total

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HIV protease inhibitors, saquinavir, indinavir and ritonavir: inhibition of CYP3A4-mediated metabolism of testosterone and benzoxazinorifamycin, KRM-1648, in human liver microsomes.

1. Rapamycin with antiretroviral therapy in AIDS-associated Kaposi sarcoma: an AIDS Malignancy Consortium study.

2. Safety and bactericidal activity of rifalazil in patients with pulmonary tuberculosis.

Review 3. Saquinavir soft-gel capsule formulation. A review of its use in patients with HIV infection.

Review 4. Optimizing HIV prevention and care for transgender adults.

5. Functional correlation of P-glycoprotein expression and genotype with expression of the human immunodeficiency virus type 1 coreceptor CXCR4.

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Review 7. Saquinavir soft gelatin capsule: a comparative safety review.

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