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Data updated: Mar 10, 2026

KALETRA

LOPINAVIR HIV Protease Inhibitors
Infectious Disease Approved 2000-09-15
13
Indications
--
Phase 3 Trials
4
Priority Reviews
25
Years on Market

Details

Status
Prescription
First Approved
2000-09-15
Routes
ORAL
Dosage Forms
TABLET, CAPSULE, SOLUTION

Companies

Active Ingredient: LOPINAVIR , RITONAVIR

KALETRA Approval History

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What KALETRA Treats

1 indications

KALETRA is approved for 1 conditions since its original approval in 2000. These indications span multiple therapeutic areas including oncology, immunology, and more.

  • HIV-1 Infection
Source: FDA Label

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Active Pipeline

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Ongoing clinical trials by development phase

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Key Completed Trials

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Completed studies with published results, ranked by significance

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Trial Timeline

Full development history with FDA approval milestones

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Understanding FDA Approval Types
Count Type What it means
- ORIG Original approval - drug first enters market
- SUPPL - Efficacy New indication (new disease/condition approved)
- SUPPL - Labeling Label text changes (warnings, dosing updates)
- SUPPL - Manufacturing Production changes (new facility)
- SUPPL - Chemistry Formulation changes (new dosage strength)

Green lines in the timeline show ORIG and Efficacy approvals - the clinically meaningful milestones.

KALETRA FDA Label Details

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Indications & Usage

FDA Label (PDF)

KALETRA is indicated in combination with other antiretroviral agents for the treatment of HIV-1 infection in adults and pediatric patients 14 days and older. Limitations of Use: Genotypic or phenotypic testing and/or treatment history should guide the use of KALETRA. The number of baseline lopinavir resistance-associated substitutions affects the virologic response to KALETRA [see Microbiology ] . KALETRA is an HIV-1 protease inhibitor indicated in combination with other antiretroviral agents for the treatment of HIV-1 infection in adults and pediatric patients (14 days and older).

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Data Sources

Data sourced from official FDA and NIH databases. Click links to verify on original sources.