Optimizing Treatment for Treatment-Experienced, HIV-Infected People

Phase 3

Completed

Conditions: HIV Infections

Interventions: Drug: Enfuvirtide
Drug: Raltegravir
Drug: Darunavir
Drug: Tipranavir
Drug: Etravirine
Drug: Maraviroc

Registration Number: NCT00537394

Lead Sponsor: National Institute of Allergy and Infectious Diseases (NIAID)

Brief Summary: The goal of anti-HIV therapy is to prevent HIV from replicating. Long-term control of HIV requires at least two anti-HIV drugs that are active against the virus. Drug resistance is a problem for many treatment-experienced, HIV-infected people. The purpose of this study was to determine the benefit of adding a nucleoside reverse transcriptase inhibitor (NRTI) to a new anti-HIV drug regimen for the suppression of HIV.

Detailed Description: Two or more fully active antiretrovirals (ARVs) are recommended for successful suppression of HIV. In people infected with resistant HIV virus, finding two drugs that are fully active against HIV can be a challenge. However, the new generation of anti-HIV drugs has been designed to suppress drug-resistant HIV. These drugs include the FDA-approved protease inhibitors (PIs) darunavir and tipranavir, the investigational non-nucleoside transcriptase inhibitor (nNRTI) etravirine, the FDA-approved fusion inhibitor enfuvirtide, the recently FDA-approved CCR5 inhibitor maraviroc, and the investigational integrase inhibitor raltegravir. Also, it is not yet known whether multiple, partially-active drugs have the same rate of success in suppressing HIV. The purpose of this study was to use HIV resistance testing to predict the potency of a suggested ARV regimen using second generation ARVs and determine if the benefits of adding NRTIs to this new drug regimen outweigh the risks of drug toxicity and pill burden. All participants had treatment experience or resistance to NRTIs, nNRTIs, and PIs, and received novel agents.

An active screening period (after enrollment but before randomization or treatment dispensation), occurred for up to 75 days for all participants, and study participation lasted an additional 96 weeks for those who qualified for either randomization or assignment (i.e. not randomized), to the study intervention. During active screening, all participants remained on their current drug regimen. During screening, phenotypic and genotypic HIV resistance tests were performed on participants' blood samples, as well as a coreceptor tropism assay. Using this information and medication history, the study team determined the best new regimen options for each participant. Each clinician, along with the study participant, then chose a new regimen based on the recommendations of the study team and the participant's preference.

Evaluation for study outcomes began when participants started their new regimen as assigned by either randomization or determined assignment. Stratification between Arms A (Add NRTIs) and B (Omit NRTIs) or Arm C (Non-randomized to Add NRTIs) was based on predicted activity of the new regimen. Those assigned to a regimen with higher predicted activity were randomly assigned to Arm A (Add NRTIs) or B (Omit NRTIs); those assigned a regimen predicted to have lower activity were not randomized, but were assigned to Arm C (Add NRTIs).

Participants in Arms A and C were instructed to take their newly assigned study regimen plus at least 2 NRTIs (personalized from expert recommendation and choice by local provider and participant) for 96 weeks. Participants in Arm B were instructed to take their newly assigned study regimen with no NRTIs for 96 weeks. Participants in all arms who met the primary efficacy outcome of regimen failure remained in the study in order to be followed for important secondary outcomes.

All participants were scheduled to have 13 clinical visits, which included blood collection. At some visits, urine collection and quality of life and adherence questionnaires occurred. A neurocognitive assessment was performed for all participants at time of starting the new study regimen. Participants may also have consented to have cerebrospinal fluid collected via lumbar puncture following study treatment assignment and/or at Week 24. Those participants who consented to cerebrospinal fluid collection also had neurocognitive assessments at the times of collections. Participants were responsible for obtaining certain ARVs not provided by the study, including the ARVs they during the active screening period.

The primary and secondary study objectives and comparisons relate to the randomized arms, and therefore, results are not provided for the non-randomized arm (C). The purpose of the non-randomized arm (C) was to include persons higher baseline resistance (and thus, lower activity scores) in order to address an exploratory objective related to the predictive power of these activity scores (and thus a larger range of scores by inclusion of arm C), on certain, virologic outcomes.

Recruitment & Eligibility

Status: COMPLETED

Sex: All

Target Recruitment: 517

Inclusion Criteria

HIV-1 infection
Triple-class drug experience or resistance. More information on this criterion can be found in the protocol.
Currently on a failing PI-containing regimen that includes 2 other ARVs with no regimen change for 8 weeks prior to study screening
HIV viral load of 1000 copies/ml or more
Hepatitis B surface antigen negative within 90 days of study entry
Able to obtain NRTIs and ritonavir and have required ARVs at time of starting study intervention
Willing to use acceptable forms of contraception
Parent or legal guardian willing to provide consent, if applicable
CD4 count result from a specimen drawn within 120 days prior to study entry
If any previous HIV-1 viral co-receptor tropism result is available, then most recent specimen date and the tropism result of that specimen AND specimen date and tropism result of any test with either X4 or D/M result, if different from the first specimen, must be available

Inclusion Criteria continued:

Receipt of successful phenotype/genotype resistance results within 105 days prior to study treatment intervention assignment
Study team identification of a study regimen and at least 2 NRTIs for participant to take
Certain abnormal laboratory values. More information on this criterion can be found in the protocol.

Exclusion Criteria

Chronic, active hepatitis B virus infection (hepatitis B surface antigen positive or HBV DNA positive)
Taking certain medications. More information on this criterion can be found in the protocol.
Known allergy/sensitivity to components of two or more of the study-provided drugs or their formulations. For maraviroc, this includes hypersensitivity or history of allergy to soy lecithin or peanuts.
Active drug or alcohol use that, in the opinion of the investigator, may interfere with the study
Pregnancy or breastfeeding
Use of any immunomodulator (interferons, interleukins, systemic corticosteroids, or cyclosporine), vaccine, or investigational therapy within 30 days prior to study treatment allocation/assignment
Require certain medications prohibited with study treatment
Serious illness requiring systemic treatment or hospitalization. Participants who complete therapy or are clinically stable on therapy for at least 14 days prior to study treatment allocation are not excluded.

Study & Design

Study Type: INTERVENTIONAL

Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
B	Tipranavir	Regimen with higher predicted activity assigned by the study without NRTIs for 96 weeks. A 3-4 drug regimen was selected from the drugs listed to the right.
B	Maraviroc	Regimen with higher predicted activity assigned by the study without NRTIs for 96 weeks. A 3-4 drug regimen was selected from the drugs listed to the right.
A	Enfuvirtide	Regimen with higher predicted activity assigned by the study plus at least 2 NRTIs (personalized choice from expert recommendation) for 96 weeks. A 3-4 drug regimen was selected from the drugs listed to the right.
A	Darunavir	Regimen with higher predicted activity assigned by the study plus at least 2 NRTIs (personalized choice from expert recommendation) for 96 weeks. A 3-4 drug regimen was selected from the drugs listed to the right.
A	Raltegravir	Regimen with higher predicted activity assigned by the study plus at least 2 NRTIs (personalized choice from expert recommendation) for 96 weeks. A 3-4 drug regimen was selected from the drugs listed to the right.
A	Tipranavir	Regimen with higher predicted activity assigned by the study plus at least 2 NRTIs (personalized choice from expert recommendation) for 96 weeks. A 3-4 drug regimen was selected from the drugs listed to the right.
A	Etravirine	Regimen with higher predicted activity assigned by the study plus at least 2 NRTIs (personalized choice from expert recommendation) for 96 weeks. A 3-4 drug regimen was selected from the drugs listed to the right.
B	Enfuvirtide	Regimen with higher predicted activity assigned by the study without NRTIs for 96 weeks. A 3-4 drug regimen was selected from the drugs listed to the right.
A	Maraviroc	Regimen with higher predicted activity assigned by the study plus at least 2 NRTIs (personalized choice from expert recommendation) for 96 weeks. A 3-4 drug regimen was selected from the drugs listed to the right.
B	Raltegravir	Regimen with higher predicted activity assigned by the study without NRTIs for 96 weeks. A 3-4 drug regimen was selected from the drugs listed to the right.
C	Enfuvirtide	Regimen with lower predicted activity assigned plus at least 2 NRTIs (personalized choice from expert recommendation) for 96 weeks. A 3-4 drug regimen was selected from the drugs listed to the right.
B	Etravirine	Regimen with higher predicted activity assigned by the study without NRTIs for 96 weeks. A 3-4 drug regimen was selected from the drugs listed to the right.
C	Raltegravir	Regimen with lower predicted activity assigned plus at least 2 NRTIs (personalized choice from expert recommendation) for 96 weeks. A 3-4 drug regimen was selected from the drugs listed to the right.
B	Darunavir	Regimen with higher predicted activity assigned by the study without NRTIs for 96 weeks. A 3-4 drug regimen was selected from the drugs listed to the right.
C	Maraviroc	Regimen with lower predicted activity assigned plus at least 2 NRTIs (personalized choice from expert recommendation) for 96 weeks. A 3-4 drug regimen was selected from the drugs listed to the right.
C	Darunavir	Regimen with lower predicted activity assigned plus at least 2 NRTIs (personalized choice from expert recommendation) for 96 weeks. A 3-4 drug regimen was selected from the drugs listed to the right.
C	Etravirine	Regimen with lower predicted activity assigned plus at least 2 NRTIs (personalized choice from expert recommendation) for 96 weeks. A 3-4 drug regimen was selected from the drugs listed to the right.
C	Tipranavir	Regimen with lower predicted activity assigned plus at least 2 NRTIs (personalized choice from expert recommendation) for 96 weeks. A 3-4 drug regimen was selected from the drugs listed to the right.

Primary Outcome Measures

Name	Time	Method
Percent of Participants With Regimen Failure, Defined as a Confirmed Virologic Failure or Discontinuation of Randomized NRTI Component of Study Treatment	From study entry to end of Week 48 evaluation window	Virologic failure defined as confirmed plasma HIV-1 RNA meeting 1 of the following 4 criteria: \< 1.0 log10 copies/mL reduction from baseline level and \>= 200 copies/mL at or after week 12 evaluation; \>= 200 copies/mL after 1 measurement \< 200 copies/mL; absence of any values \< 200 copies/mL by and including week 24 evaluation; \>= 200 copies/mL at week 48 evaluation. Discontinuation of Randomized NRTI component of Study Treatment is defined as permanently stopping all NRTIs among those randomized to add NRTIs, or starting any NRTI among those randomized to omit NRTIs. Subjects leaving the study for reasons other than death, relocation, incarceration, or site closure were reviewed for the discontinuation outcome by a blinded, independent panel. Additionally, any participant failing to start study treatment after randomization and prior to closure was also reviewed. Results report percent of participants reaching regimen failure outcome by week 48 evaluation using Kaplan-Meier method.

Secondary Outcome Measures

Name	Time	Method
Time From Treatment Dispensation to First Study ARV Modification (Excluding NRTIs, if Applicable)	From treatment dispensation to week 96 study visit	First study ARV modification included any discontinuation or substitution of any chosen and initiated ARV for any reason. Events prompting study medication change could include protocol required (e.g. safety), protocol recommended but not required (e.g. virologic failure), or participant motivated (such as non-adherence, loss to follow-up or death; in other words, not protocol recommended or required). Event times were the exact weeks from treatment initiation to the time of qualifying regimen modification. Censoring times were the exact weeks from treatment initiation to the last date of study drugs. The week 96 (final study visit) could occur up through 110 weeks following randomization.
Number of Participants With Plasma HIV-1 Viral Load < 50 Copies/ml	At Weeks 24, 48, 96	Number of participants with plasma HIV-1 Viral load \< 50 copies/mL at study visit weeks 24, 48, and 96. Closest observed result between 20 and up to 30 weeks (for week 24), between 42 and up to 54 (for week 48), and between 90 and up to 110 (for week 96) used if multiple results available. Missing values excluded.
Change in Plasma HIV-1 Viral Load From Baseline to Week 1	From baseline to Week 1 evaluation	Method of Kaplan and Meier used to accommodate left-censoring for those whose week 1 levels \< 50 copies/mL.
Change in Summarized Quality of Life Score	At study entry and Weeks 24, 48, 96	Quality-of-life score at each evaluation based upon a single question assessing participants' self-report of general health with a range of 0 (representing worst health status) to 100 (representing perfect health).
Number of Participants Self-reporting Non-adherence to Assigned Study ARVS (Excluding NRTIs, if Applicable)	At Weeks 24 and 48	Results represent self-report of non-adherence during the 4-day period prior to the outcome evaluation visit. Participants in follow-up for whom these data are missing for any reason are inferred as not-adherent.
Time From Treatment Dispensation to First Grade 3 or Higher (and at Least One Grade Higher Than Baseline) Signs/Symptom or Laboratory Abnormality	From treatment dispensation to week 96 study visit	Events following permanent discontinuation of NRTI assignment are excluded (i.e. censoring at time of this event, if applicable). Week 96 study visit could occur up to 110 weeks following randomization. Censoring time was the latest study visit when participant was evaluated or when NRTI assignment was discontinued (when applicable). Event time was the exact number of weeks following treatment initiation when the qualifying sign/symptom started (for those safety events triggered by a sign/symptom), or exact number of weeks following treatment initiation when specimen from qualifying laboratory result was drawn (for those safety events triggered by a laboratory abnormality).
Time From Randomization to Confirmed Virological Failure	From randomization to week 96 study visit	Virologic failure defined as confirmed (two consecutive) plasma HIV-1 RNA meeting 1 of the following 4 criteria: \< 1.0 log10 copies/mL reduction from baseline level and \>= 200 copies/mL at or after week 12 evaluation; \>= 200 copies/mL after 1 measurement \< 200 copies/mL; absence of any values \< 200 copies/mL by and including week 24 evaluation; \>= 200 copies/mL at week 48 evaluation. Event time was the scheduled study visit week when the initial plasma HIV-1 RNA specimen meeting the failure definition was collected. Censoring time was the latest scheduled study visit week when a plasma HIV-1 RNA specimen was collected and tested.
Change in CD4 Count From Baseline	From study entry to Weeks 48 and 96	Baseline CD4 calculated as average of pre-entry and entry values. Closest observed result between 42 and up to 54 weeks (for week 48) or between 90 and up to 110 weeks (for week 96), used if multiple results available. Missing values excluded.
Change in Fasting Non-HDL Cholesterol From Baseline	From study entry to Weeks 24, 48	Fasting non-HDL cholesterol calculated from difference between fasting total cholesterol and fasting HDL level. Missing values and non-fasting values excluded.
Participants With Newly Acquired HIV Drug Resistance Between Study Entry and Confirmed Virologic Failure	Between baseline and confirmed virologic failure (up to 96 weeks)	Defined among the subgroup of participants experiencing the outcome of confirmed virologic failure. Newly acquired HIV drug resistance is defined as one or more ARVs with partial resistance or resistance when pre-entry resistance was fully sensitive or resistant when pre-entry resistance was fully sensitive or partially sensitive. The ARVs included for resistance acquisition included the following: darunavir/ritonavir; etravirine, tipranavir, tenofovir, emtracitabine, lamivudine, zidovudine, abacavir.
Time From Randomization to Discontinuation of Randomized NRTI Component of Study Treatment	From randomization to week 96 study visit	Discontinuation of Randomized NRTI component of Study Treatment is defined as permanently stopping all NRTIs among those randomized to add NRTIs, or starting any NRTI among those randomized to omit NRTIs. Subjects leaving the study for reasons other than death, relocation, incarceration, or site closure were reviewed for meeting this outcome by a blinded, independent panel. Additionally, any participant failing to start study treatment after randomization and prior to closure was also reviewed. Event times were scheduled study weeks when discontinuation events occurred. Censoring times were latest scheduled study visit weeks with evaluation.
Time From Treatment Dispensation to Serious Non-AIDS-defining Events	From treatment initiation to week 96 study visit	Serious Non-AIDS defining Events were adjudicated by independent and blinded review and possible events included serious diagnoses in the following disease areas: liver, cardiovascular, end-stage renal, non-AIDS malignancy, and diabetes mellitus. Week 96 study visit could take place up to 110 weeks following randomization. Event times were the exact weeks following treatment initiation corresponding to the diagnosis dates of the qualifying serious non-AIDS defining events. Censoring times were the weeks following treatment initiation corresponding to the latest study visit.
Number of Participants With Change in Virus Co-receptor Tropism Among Those With R5-only Tropic Virus at Study Entry	From study entry to time of confirmed virological failure (up to 96 weeks)	HIV Co-receptor tropism test result of either dual/mixed or evidence of X4 using virus from sample collected at confirmed virologic failure.
Change in Cardiovascular Risk Score From Baseline	At Weeks 24, 48, and 96	Cardiovascular risk score defined by Framingham providing an estimate of the probability of developing cardiovascular disease over the next 10-year period. Persons with a historical cardiovascular event (CAD, cerebro- or peripheral- vascular disorder, MI or stroke), were excluded, and scores were not calculated at follow-up times after individuals had a cardiovascular event. Missing values for input data (e.g. smoking status) resulted in a missing value for Framingham score.

Trial Locations

Locations (64): Children's National Med. Ctr. ATN CRS
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Washington, District of Columbia, United States
Univ. of Rochester ACTG CRS
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Rochester, New York, United States
UCLA CARE Center CRS
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Los Angeles, California, United States
The Ponce de Leon Center CRS
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Atlanta, Georgia, United States
Boston Medical Center Ped. HIV Program NICHD CRS
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Boston, Massachusetts, United States
Northwestern University CRS
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Chicago, Illinois, United States
Cincinnati CRS
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Cincinnati, Ohio, United States
Case Clinical Research Site
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Cleveland, Ohio, United States
MetroHealth CRS
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Cleveland, Ohio, United States
Ohio State University CRS
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Columbus, Ohio, United States
Penn Therapeutics, CRS
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Philadelphia, Pennsylvania, United States
Trinity Health and Wellness Center CRS
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Dallas, Texas, United States
Houston AIDS Research Team CRS
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Houston, Texas, United States
Texas Children's Hospital CRS
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Houston, Texas, United States
University of Southern California CRS
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Los Angeles, California, United States
Miller Children's Hosp. Long Beach CA NICHD CRS
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Long Beach, California, United States
Stanford AIDS Clinical Trials Unit CRS
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Palo Alto, California, United States
Ucsf Hiv/Aids Crs
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San Francisco, California, United States
Univ. of California San Francisco NICHD CRS
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San Francisco, California, United States
University of Colorado Hospital CRS
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Aurora, Colorado, United States
Denver Public Health CRS
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Denver, Colorado, United States
Georgetown University CRS (GU CRS)
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Washington, District of Columbia, United States
Rush University CRS
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Chicago, Illinois, United States
Johns Hopkins University CRS
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Baltimore, Maryland, United States
Bronx-Lebanon Hosp. Ctr. CRS
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Bronx, New York, United States
NY Univ. HIV/AIDS CRS
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New York, New York, United States
Weill Cornell Chelsea CRS
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New York, New York, United States
Nyu Ny Nichd Crs
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New York, New York, United States
Columbia P&S CRS
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New York, New York, United States
Columbia IMPAACT CRS
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New York, New York, United States
Alabama Therapeutics CRS
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Birmingham, Alabama, United States
Wayne State Univ. CRS
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Detroit, Michigan, United States
Henry Ford Hosp. CRS
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Detroit, Michigan, United States
IHV Baltimore Treatment CRS
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Baltimore, Maryland, United States
Bmc Actg Crs
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Boston, Massachusetts, United States
Beth Israel Deaconess Med. Ctr., ACTG CRS
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Boston, Massachusetts, United States
Howard Univ. Washington DC NICHD CRS
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Washington, District of Columbia, United States
The Research & Education Group-Portland CRS
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Portland, Oregon, United States
Pediatric Perinatal HIV Clinical Trials Unit CRS
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Miami, Florida, United States
New Jersey Medical School Clinical Research Center CRS
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Newark, New Jersey, United States
Tulane Univ. New Orleans NICHD CRS
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New Orleans, Louisiana, United States
Cooper Univ. Hosp. CRS
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Camden, New Jersey, United States
Massachusetts General Hospital CRS (MGH CRS)
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Boston, Massachusetts, United States
Brigham and Women's Hospital Therapeutics Clinical Research Site (BWH TCRS) CRS
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Boston, Massachusetts, United States
Rutgers - New Jersey Medical School CRS
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Newark, New Jersey, United States
Vanderbilt Therapeutics (VT) CRS
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Nashville, Tennessee, United States
San Juan City Hosp. PR NICHD CRS
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San Juan, Puerto Rico
Puerto Rico AIDS Clinical Trials Unit CRS
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San Juan, Puerto Rico
University of Puerto Rico Pediatric HIV/AIDS Research Program CRS
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San Juan, Puerto Rico
St. Jude Children's Research Hospital CRS
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Memphis, Tennessee, United States
Usc La Nichd Crs
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Los Angeles, California, United States
UCLA-Los Angeles/Brazil AIDS Consortium (LABAC) CRS
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Los Angeles, California, United States
UCSD Antiviral Research Center CRS
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San Diego, California, United States
Metropolitan Hosp. NICHD CRS
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New York, New York, United States
Harlem ACTG CRS
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New York, New York, United States
Trillium Health ACTG CRS
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Rochester, New York, United States
Chapel Hill CRS
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Chapel Hill, North Carolina, United States
Duke Univ. Med. Ctr. Adult CRS
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Durham, North Carolina, United States
Thomas Jefferson Univ. Med. Ctr. CRS
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Philadelphia, Pennsylvania, United States
University of Pittsburgh CRS
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Pittsburgh, Pennsylvania, United States
The Miriam Hospital Clinical Research Site (TMH CRS) CRS
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Providence, Rhode Island, United States
Virginia Commonwealth Univ. Medical Ctr. CRS
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Richmond, Virginia, United States
University of Washington AIDS CRS
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Seattle, Washington, United States
Washington University Therapeutics (WT) CRS
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Saint Louis, Missouri, United States