Switch to Unboosted Atazanavir With Tenofovir Study

Phase 4

Completed

• Conditions: HIV Infection
• Interventions: Drug: atazanavir/ritonavir; Drug: atazanavir

• Registration Number: NCT01351740
• Lead Sponsor: University of British Columbia

Brief Summary

A drug-drug interaction between the anti-HIV drugs tenofovir DF (TDF) and atazanavir (ATZ) results in lower ATZ plasma levels when the drugs are given together, particularly in patients not taking ritonavir to boost ATZ levels. Lower plasma drug levels may make the anti-HIV regimen less effective in controlling the HIV virus levels in the blood. For this reason, current treatment guidelines recommend that ATZ always be boosted with ritonavir in regimens also containing TDF. However, withdrawal of ritonavir is often desirable given the tolerability and toxicity issues with this agent, even at the low dose (100 mg daily) used to boost ATZ. For example, ritonavir can cause stomach upset, nausea, diarrhea, high cholesterol levels, and liver enzyme abnormalities.

However, there is evidence that plasma ATZ levels may not predict treatment success on unboosted ATZ regimens, particularly among people whose plasma HIV virus is already under control and unboosted ATZ is being used as a maintenance strategy. In the BC Centre for Excellence in HIV/AIDS Drug Treatment Program (DTP), nearly 100 patients originally treated with ritonavir-boosted ATZ + TDF (+ FTC or 3TC) are receiving successful maintenance therapy with unboosted ATZ and the same TDF-based backbone.

The study will examine the hypothesis that switching to maintenance therapy with unboosted ATZ 400mg daily will have similar 48-week virologic efficacy to continuing ATZ/ritonavir 300/100mg daily among HIV-infected adults with stable viral load suppression on regimens comprising ATZ/ritonavir 300/100mg daily with TDF plus either FTC or 3TC, despite potentially lower ATZ trough levels with the unboosted regimen. In other words, patients whose HIV viral load is undetectable while receiving TDF (+FTC or 3TC) and ATZ/ritonavir will continue to maintain an undetectable viral load after switching to unboosted ATZ without ritonavir, in the same proportions as those continuing on their boosted ATZ/ritonavir regimen.

Detailed Description

Following a screening visit to establish study eligibility, eligible consenting subjects will be randomized 1:1 to one of the two treatment arms (switch to unboosted ATZ or continue ritonavir-boosted ATZ). Randomized open-label treatment will commence following study procedures at baseline. Participants will be assessed at baseline and at weeks 4, 8, 12, 24, 36, and 48. On-study evaluations will include assessment of adverse clinical events and medication changes; blood tests for HIV viral load, CD4 cell count, standard safety parameters, fasting lipids and glucose, and pregnancy testing (if applicable); and urine tests for urinalysis and albumin to creatinine ratio. In addition, a serum sample will be stored at each visit for possible future testing. A timed plasma sample for measurement of pre-dose trough ATZ levels will be obtained once per subject at 4-8 weeks. Quality of life will be assessed by completion of the MOS-HIV questionnaire at baseline and every 12 weeks. Adherence will be assessed based on prescription refill data.

In case of protocol-defined virologic failure, a plasma sample for ATZ trough level will be collected, and genotypic resistance testing will be performed on plasma samples with viral load \>250 copies/mL. Subjects with confirmed virologic failure will be asked to come to the clinic and will have their HIV treatment changed to a more effective regimen, selected based on the results of genotypic testing, as soon as possible.

The anticipated rate of confirmed virologic failure in the control arm is no more than 15% over the 48 weeks of the study. Once at least 20 subjects have been assigned to the experimental (switch) treatment arm, if the observed confirmed virologic failure rate in the experimental arm is greater than twice this rate, i.e. \>30%, at any time during the study, the study will be stopped. At this time, subjects in the experimental arm will be reassessed as soon as possible and will resume ritonavir-boosted atazanavir or other effective HIV therapy as appropriate. The failure rate will be reassessed at a minimum after each 20 subjects are enrolled into the experimental (switch) arm.

Study Timeline

• Study First Submitted: 2011-05-09
• Study First Submitted QC: 2011-05-10
• Study First Posted: 2011-05-11
• Study Start: 2011-07
• Primary Completion: 2015-01
• Study Completion: 2015-12
• Status Verified: 2017-10
• Results First Submitted: 2017-10-24
• Results First Submitted QC: 2017-10-24
• Last Update Submitted: 2017-10-24
• Results First Posted: 2018-07-30
• Last Update Posted: 2018-07-30

Recruitment & Eligibility

• Status: COMPLETED
• Sex: All
• Target Recruitment: 50

Inclusion Criteria

1. HIV infected adults at least 19 years of age
2. Willing and able to provide informed consent to study participation
3. Currently receiving a regimen including atazanavir 300mg/ritonavir 100mg daily with either tenofovir/emtricitabine (FTC) or tenofovir/lamivudine (3TC), for at least 3 months
4. Plasma viral load (VL) <40 copies/mL for at least 2 consecutive measurements including the screening value, and < 150 copies/mL continuously for at least 3 months prior to screening
5. Current regimen is first antiretroviral regimen, or if not first regimen, no evidence of resistance to any nucleosides (NRTIs) or protease inhibitors (PIs) on previous resistance tests
6. Any CD4

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Exclusion Criteria

1. Clinically significant intolerance or toxicity with current regimen precluding regimen continuation (e.g. intolerance/toxicity to ritonavir necessitating ritonavir discontinuation)
2. pregnancy or breast-feeding
3. antiretroviral regimen including any nonnucleoside reverse transcriptase inhibitor (nevirapine, efavirenz, or etravirine)
4. antiretroviral regimen including any protease inhibitor other than atazanavir and ritonavir
5. concomitant treatment with proton pump inhibitors, rifampin, St. John's wort, or garlic supplements. (Antacids and H2 receptor antagonists will be allowed provided their dosing is separated from atazanavir administration by at least 2 and 10 hours, respectively).

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Study & Design

• Study Type: INTERVENTIONAL
• Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
Continuation	atazanavir/ritonavir	continue on current regimen of atazanavir/ritonavir 300mg/100mg with the same nucleoside (NRTI) backbone
Switch	atazanavir	switch to unboosted atazanavir 400mg daily with the same nucleoside (NRTI) backbone

Primary Outcome Measures

Name	Time	Method
Proportions of Subjects Experiencing Virologic Failure by Randomized Treatment Arm	at or before 48 weeks.	For the purposes of the study, virologic failure is defined as either regimen change for any reason, or plasma viral load \>400 copies/mL on 2 consecutive measurements \>2 weeks apart.

Secondary Outcome Measures

Name	Time	Method
Proportions of Subjects in Each Randomized Treatment Arm With Atazanavir Trough Levels Below 150ng/mL	1 month (4-8 weeks)	Therapeutic drug monitoring (TDM) to determine atazanavir trough plasma level will be performed once on all subjects at 4-8 weeks
Proportion of Subjects Experiencing Virologic Failure by Results of 1-month TDM	at or before 24 weeks	For the purposes of the study, virologic failure is defined as either regimen change for any reason, or plasma viral load \>400 copies/mL on 2 consecutive measurements \>2 weeks apart. Comparison will be made between subjects with 1-month (4-8 week) on-study atazanavir trough levels \<150ng/mL and those with 1-month (4-8 week) on-study atazanavir trough levels \>150ng/mL.
Proportions of Subjects Experiencing Virologic Failure by Randomized Treatment Arm	at or before 24 weeks.	For the purposes of the study, virologic failure is defined as either regimen change for any reason, or plasma viral load \>400 copies/mL on 2 consecutive measurements \>2 weeks apart.
CD4 Cell Count Changes (Absolute and Fraction)	24 and 48 weeks	Comparison will be made between randomized treatment arms.
Safety (Clinical and Laboratory Adverse Events)	24 and 48 weeks	Serious adverse events and discontinuations will be compared between randomized treatment arms
Total Serum Bilirubin Levels	24 and 48 weeks	Comparison will be made between randomized treatment arms.
Metabolic Parameters	24 and 48 weeks	Comparison will be made between randomized treatment arms with respect to changes in fasting lipids and glucose, highly sensitive C-reactive protein \[hsCRP\], and apolipoprotein \[apo\]B, and proportions of subjects developing abnormalities or crossing predefined limits (e.g. NCEP thresholds for lipids)
Quality of Life as Assessed by MOS-HIV	24 and 48 weeks	Changes in MOS-HIV scores from baseline will be compared between randomized treatment arms.

Trial Locations

Locations (1)

Immunodeficiency Clinic, St. Paul's Hospital; 🇨🇦 Vancouver, British Columbia, Canada