Study to Evaluate a HIV Drug for the Treatment of HIV Infection

Phase 2

Completed

Conditions: Infection, Human Immunodeficiency Virus
HIV Infections

Interventions: Drug: Atazanavir
Drug: BMS-955176
Drug: Placebo matching with BMS-955176
Drug: Tenofovir
Drug: Ritonavir
Drug: Emtricitabine

Registration Number: NCT01803074

Lead Sponsor: ViiV Healthcare

Brief Summary: The primary purpose of this study is to study the safety and tolerability of a HIV drug and to evaluate a decrease of HIV-1 virus level in blood after treatments in HIV-1 infected patients

Detailed Description: Masking: Open-Part B. Double Blind-Parts A and C

Gender: Both female and male participants for Parts A and C. Male participants for Part B.

HIV = Human Immunodeficiency Virus RNA = Ribonucleic acid

Recruitment & Eligibility

Status: COMPLETED

Sex: All

Target Recruitment: 107

Inclusion Criteria

Age 18-55 years inclusive
Men and women: (Parts A and C); men only (Part B)
Women of childbearing potential (WOCBP) must not be pregnant and nursing
BMI: 18.0-35.0 kg/m2
Subjects are infected with HIV-1 (clades B or C) and meet following criteria at the screening:

i) Plasma HIV-1 RNA ≥5,000 copies/mL; ii) Antiretroviral treatment naive (defined as <1 week of ARV treatment) or ART-experienced (protease inhibitor and/or maturation inhibitor naive); iii) Subjects are not eligible for HIV-1 treatment based on the United States Department of Health and Human Services Panel on Antiretroviral Guidelines for Adults and Adolescents or have declined initiation of cART iv) CD4+ lymphocyte measurement ≥200 cells/μL; v) In Parts A and B, all subjects are infected with HIV-1 clade B vi) In Part C, all subjects are infected with HIV-1 clade C

Exclusion Criteria

History of genotypic and/or phenotypic drug resistance testing showing resistance to protease inhibitors
Any significant acute or chronic medical illness which is not stable or is not controlled with medication or not consistent with HIV-1 infection
Receive antiretroviral treatment within 12 weeks prior to screening
Currently co-infected with hepatitis C or hepatitis B
Previously received an HIV maturation inhibitor or HIV protease inhibitor
Current or recent (within 3 months of study drug administration) gastrointestinal disease
Any major surgery within 4 weeks of study drug administration
Acute diarrhea lasting ≥1 day, within 3 weeks prior to randomization
Subjects with history of Gilbert's syndrome
Subjects previously received an HIV maturation inhibitor or HIV protease inhibitor
A personal history of clinically relevant cardiac disease, symptomatic or asymptomatic arrhythmias, syncopal episodes, or additional risk factors for torsades de pointes. A personal or family history of long QT syndrome
Patients who are unwilling to practice adequate infection protection during and after study participation to minimize potential for spread of HIV infection, including HIV which may have developed resistance to HIV maturation inhibitor and/or ATV
Any gastrointestinal surgery that could impact upon the absorption of study drug
Smoking >10 cigarettes per day
PR ≥210 msec; QRS ≥120 msec; QT ≥500 msec; and QTcF ≥470 msec for women and ≥450 msec for men
Evidence of second or third degree heart block prior to study drug
Absolute Neutrophil Count <(ANC) 0.7 x lower limit of normal (LLN)
Hemoglobin <0.8 x LLN
Alanine aminotransferase (ALT) >1.25 x upper limit of normal (ULN)
Aspartate aminotransferase (AST) >1.25 x ULN
Total Bilirubin >1.25 x ULN
Creatinine clearance <60 mL/mim
Positive urine screen for drugs of abuse without a valid prescription (subjects positive for cannabinoids and/or amphetamines will be included)
Positive blood screen for hepatitis C virus (HCV) RNA, hepatitis B surface antigen (consistent with active or chronic hepatitis B), or HIV-2 antibody
History of any significant drug allergy

Study & Design

Study Type: INTERVENTIONAL

Study Design: PARALLEL

Arm && Interventions

Group	Intervention	Description
Part B-Group 7: Atazanavir+Ritonavir+Tenofovir+Emtricitabine	Tenofovir	Atazanavir 1 x 300 mg capsule by mouth once daily for 28 days Ritonavir 1 x 100 mg tablet by mouth once daily for 28 days Tenofovir 1 x 300 mg tablet by mouth once daily for 28 days Emtricitabine 1 x 200 mg capsule once daily for 28 days
Part A-Group 1: BMS-955176 (5 mg) or Placebo	Placebo matching with BMS-955176	BMS-955176 5 mg solution by mouth once daily for 10 days OR Placebo matching with BMS-955176 0 mg solution by mouth once daily for 10 days
Part A-Group 2: BMS-955176 (10 mg) or Placebo	Placebo matching with BMS-955176	BMS-955176 10 mg solution by mouth once daily for 10 days OR Placebo matching with BMS-955176 0 mg solution by mouth once daily for 10 days
Part A-Group 3: BMS-955176 (20 mg) or Placebo	Placebo matching with BMS-955176	BMS-955176 20 mg solution by mouth once daily for 10 days OR Placebo matching with BMS-955176 0 mg solution by mouth once daily for 10 days
Part A-Group 4: BMS-955176 (40 mg) or Placebo	Placebo matching with BMS-955176	BMS-955176 40 mg solution by mouth once daily for 10 days OR Placebo matching with BMS-955176 0 mg solution by mouth once daily for 10 days
Part B-Group 7: Atazanavir+Ritonavir+Tenofovir+Emtricitabine	Atazanavir	Atazanavir 1 x 300 mg capsule by mouth once daily for 28 days Ritonavir 1 x 100 mg tablet by mouth once daily for 28 days Tenofovir 1 x 300 mg tablet by mouth once daily for 28 days Emtricitabine 1 x 200 mg capsule once daily for 28 days
Part C-Group 8: BMS-955176 (40 mg) or Placebo	Placebo matching with BMS-955176	BMS-955176 40 mg solution by mouth once daily for 10 days OR Placebo matching with BMS-955176 0 mg solution by mouth once daily for 10 days
Part A-Group 9: BMS-955176 (80 mg) or Placebo	Placebo matching with BMS-955176	BMS-955176 80 mg solution by mouth once daily for 10 days OR Placebo matching with BMS-955176 0 mg solution by mouth once daily for 10 days
Part A-Group 10: BMS-955176 (120 mg) or Placebo	Placebo matching with BMS-955176	BMS-955176 120 mg solution by mouth once daily for 10 days OR Placebo matching with BMS-955176 0 mg solution by mouth once daily for 10 days
Part A-Group 11 (Optional): BMS-955176 (≤120 mg) or Placebo	Placebo matching with BMS-955176	BMS-955176 ≤120 mg solution by mouth once daily for 14 days OR Placebo matching with BMS-955176 0 mg solution by mouth once daily for 14 days
Part B-Group 12: BMS-955176 (80 mg) + Atazanavir	BMS-955176	BMS-955176 80 mg solution by mouth once daily for 28 days Atazanavir 2 x 200 mg capsules by mouth once daily for 28 days
Part B-Group 12: BMS-955176 (80 mg) + Atazanavir	Atazanavir	BMS-955176 80 mg solution by mouth once daily for 28 days Atazanavir 2 x 200 mg capsules by mouth once daily for 28 days
Part C-Group 13: BMS-955176 (120 mg) or Placebo	BMS-955176	BMS-955176 120 mg solution by mouth once daily for 10 days OR Placebo matching with BMS-955176 0 mg solution by mouth once daily for 10 days
Part C-Group 13: BMS-955176 (120 mg) or Placebo	Placebo matching with BMS-955176	BMS-955176 120 mg solution by mouth once daily for 10 days OR Placebo matching with BMS-955176 0 mg solution by mouth once daily for 10 days
Part B-Group 5: BMS-955176 + Atazanavir	BMS-955176	BMS-955176 40 mg solution by mouth once daily for 28 days Atazanavir 2 x 200 mg capsules by mouth once daily for 28 days
Part A-Group 2: BMS-955176 (10 mg) or Placebo	BMS-955176	BMS-955176 10 mg solution by mouth once daily for 10 days OR Placebo matching with BMS-955176 0 mg solution by mouth once daily for 10 days
Part A-Group 3: BMS-955176 (20 mg) or Placebo	BMS-955176	BMS-955176 20 mg solution by mouth once daily for 10 days OR Placebo matching with BMS-955176 0 mg solution by mouth once daily for 10 days
Part A-Group 4: BMS-955176 (40 mg) or Placebo	BMS-955176	BMS-955176 40 mg solution by mouth once daily for 10 days OR Placebo matching with BMS-955176 0 mg solution by mouth once daily for 10 days
Part B-Group 5: BMS-955176 + Atazanavir	Atazanavir	BMS-955176 40 mg solution by mouth once daily for 28 days Atazanavir 2 x 200 mg capsules by mouth once daily for 28 days
Part B-Group 6: BMS-955176 + Atazanavir + Ritonavir	Atazanavir	BMS-955176 40 mg solution by mouth once daily for 28 days Atazanavir 1 x 300 mg capsules by mouth once daily for 28 days Ritonavir 1 x 100 mg tablet by mouth once daily for 28 days
Part B-Group 6: BMS-955176 + Atazanavir + Ritonavir	Ritonavir	BMS-955176 40 mg solution by mouth once daily for 28 days Atazanavir 1 x 300 mg capsules by mouth once daily for 28 days Ritonavir 1 x 100 mg tablet by mouth once daily for 28 days
Part B-Group 7: Atazanavir+Ritonavir+Tenofovir+Emtricitabine	Ritonavir	Atazanavir 1 x 300 mg capsule by mouth once daily for 28 days Ritonavir 1 x 100 mg tablet by mouth once daily for 28 days Tenofovir 1 x 300 mg tablet by mouth once daily for 28 days Emtricitabine 1 x 200 mg capsule once daily for 28 days
Part B-Group 7: Atazanavir+Ritonavir+Tenofovir+Emtricitabine	Emtricitabine	Atazanavir 1 x 300 mg capsule by mouth once daily for 28 days Ritonavir 1 x 100 mg tablet by mouth once daily for 28 days Tenofovir 1 x 300 mg tablet by mouth once daily for 28 days Emtricitabine 1 x 200 mg capsule once daily for 28 days
Part A-Group 10: BMS-955176 (120 mg) or Placebo	BMS-955176	BMS-955176 120 mg solution by mouth once daily for 10 days OR Placebo matching with BMS-955176 0 mg solution by mouth once daily for 10 days
Part A-Group 1: BMS-955176 (5 mg) or Placebo	BMS-955176	BMS-955176 5 mg solution by mouth once daily for 10 days OR Placebo matching with BMS-955176 0 mg solution by mouth once daily for 10 days
Part B-Group 6: BMS-955176 + Atazanavir + Ritonavir	BMS-955176	BMS-955176 40 mg solution by mouth once daily for 28 days Atazanavir 1 x 300 mg capsules by mouth once daily for 28 days Ritonavir 1 x 100 mg tablet by mouth once daily for 28 days
Part C-Group 8: BMS-955176 (40 mg) or Placebo	BMS-955176	BMS-955176 40 mg solution by mouth once daily for 10 days OR Placebo matching with BMS-955176 0 mg solution by mouth once daily for 10 days
Part A-Group 11 (Optional): BMS-955176 (≤120 mg) or Placebo	BMS-955176	BMS-955176 ≤120 mg solution by mouth once daily for 14 days OR Placebo matching with BMS-955176 0 mg solution by mouth once daily for 14 days
Part A-Group 9: BMS-955176 (80 mg) or Placebo	BMS-955176	BMS-955176 80 mg solution by mouth once daily for 10 days OR Placebo matching with BMS-955176 0 mg solution by mouth once daily for 10 days

Primary Outcome Measures

Name	Time	Method
Change in Plasma Log10 HIV-1 Ribonucleic Acid (RNA) Levels From Baseline to Day 11	Baseline (Day 1) and Day 11 after the final dose with BMS-955176	Antiviral activity of BMS-955176 was estimated by measuring the plasma HIV-1 RNA levels in the HIV-1 infected participants. Change in the plasma HIV-1 RNA levels were measured in the participants infected with HIV-1 clade B and C who received BMS-955176 monotherapy. Baseline was Day 1. Change from Baseline was post-Baseline individual values minus Baseline values.

Secondary Outcome Measures

Name	Time	Method
Time to Reach Maximum Plasma Concentration (Tmax) - Part A and C	Pre-dose Day 1 and Day 10	Time to reach the maximum plasma concentration was directly determined from concentration time data.
Number of Participants With Death as Outcome, Serious Adverse Events (SAEs), Related SAEs, Discontinuations Due to SAEs, Adverse Events (AEs), and Discontinuations Due to AEs During the Study	Day 1 to end of the study (Day 42)	AE=any new unfavorable symptom, sign, or disease or worsening of a preexisting condition that may not have a causal relationship with treatment. SAE=a medical event that at any dose results in death, persistent or significant disability/incapacity, or drug dependency/abuse; is life-threatening, an important medical event, or a congenital anomaly/birth defect; or requires or prolongs hospitalization. Related=having certain, probable, possible, or unknown relationship to study drug.
Maximum Decline From Baseline in Log10 HIV-1 RNA - Part A and C	Baseline (Day 1) up to Day 24	Antiviral activity of BMS-955176 was estimated by measuring the plasma HIV-1 RNA levels in the HIV-1 infected participants. Maximum decline from Baseline in the plasma HIV-1 RNA levels were measured in the participants infected with HIV-1 clade B and C. Baseline was Day 1. Change from Baseline was post-Baseline individual values minus Baseline values.
Maximum Decline From Baseline in Log10 HIV-1 RNA - Part B	Baseline (Day 1) up to Day 42	Antiviral activity of BMS-955176 was estimated by measuring the plasma HIV-1 RNA levels in the HIV-1 infected participants. Maximum decline from Baseline in the plasma HIV-1 RNA levels were measured in the participants infected with HIV-1 clade B and C. Baseline was Day 1. Change from Baseline was post-Baseline individual values minus Baseline values.
Time to Maximum Decline in Log 10 HIV-1 RNA - Part A and C	Baseline (Day 1) up to Day 24	Antiviral activity of BMS-955176 was estimated by measuring the plasma HIV-1 RNA levels in the HIV-1 infected participants. Time to maximum decline in the plasma HIV-1 RNA levels were measured in the participants infected with HIV-1 clade B and C. Baseline was Day 1. Change from Baseline was post-Baseline individual values minus Baseline values.
Time to Maximum Decline in Log 10 HIV-1 RNA - Part B	Baseline (Day 1) up to Day 42	Antiviral activity of BMS-955176 was estimated by measuring the plasma HIV-1 RNA levels in the HIV-1 infected participants. Time to maximum decline in the plasma HIV-1 RNA levels were measured in the participants infected with HIV-1 clade B and C. Baseline was Day 1. Change from Baseline was post-Baseline individual values minus Baseline values.
Change From Baseline in Cluster of Differentiation (CD) 4+ and CD8+ Lymphocyte Counts - Part A and C	Baseline (Day 1) up to Day 24	Change in the CD4+ and CD8+ cell counts from Baseline were measured in the participants infected with HIV-1 clade B and C who received BMS-955176 + ATV or BMS-955176 + ATV + RTV therapy. Baseline was Day 1. Change from Baseline was post-Baseline individual values minus Baseline values.
Change From Baseline in Cluster of Differentiation (CD) 4+ and CD8+ Lymphocyte Counts - Part B	Baseline (Day 1) up to Day 42	Change in the CD4+ and CD8+ cell counts from Baseline were measured in the participants infected with HIV-1 clade B and C who received BMS-955176 + ATV or BMS-955176 + ATV + RTV therapy. Baseline was Day 1. Change from Baseline was post-Baseline individual values minus Baseline values.
Percent Change From Baseline in Cluster of Differentiation (CD) 4+ and CD8+ Lymphocyte Percent - Part A and C	Baseline (Day 1) up to Day 24	Percent Change in the CD4+ and CD8+ cell counts from Baseline were measured in the participants infected with HIV-1 clade B and C who received BMS-955176 + ATV or BMS-955176 + ATV + RTV therapy. Baseline was Day 1. Change from Baseline was post-Baseline individual values minus Baseline values.
Percent Change From Baseline in Cluster of Differentiation (CD) 4+ and CD8+ Lymphocyte Percent - Part B	Baseline (Day 1) up to Day 42	Percent Change in the CD4+ and CD8+ cell counts from Baseline were measured in the participants infected with HIV-1 clade B and C who received BMS-955176 + ATV or BMS-955176 + ATV + RTV therapy. Baseline was Day 1. Change from Baseline was post-Baseline individual values minus Baseline values.
Time to Reach Maximum Plasma Concentration (Tmax) - Part B	Pre-dose Day 1 and Day 28	Tmax was directly determined from concentration time data.
Maximum Observed Plasma Concentrations (Cmax) - Part A and C	Pre-dose Day 1 and Day 10	Cmax was defined as the peak plasma concentration of a drug after administration, obtained directly from the plasma concentration-time curve.
Plasma Concentration 24 Hours Post-Dose (C24) - Part A and C	24 hours post-dose	C24 was defined as the plasma concentration of BMS-955176 at 24 hours post-dose.
Maximum Observed Plasma Concentrations (Cmax) - Part B	Pre-dose Day 1 and Day 28	Cmax was defined as the peak plasma concentration of a drug after administration, obtained directly from the plasma concentration-time curve.
Plasma Concentration 24 Hours Post-Dose (C24) - Part B	24 hours post-dose	C24 was defined as the plasma concentration of BMS-955176 at 24 hours post-dose.
Area Under The Plasma Concentration - Time Curve Over the Dosing Interval (AUC([Tau]) - Part A and C	Pre-dose Day 1 and Day 10	AUC(tau) was defined as the area under the plasma concentration - time curve over the dosing interval.
Area Under The Plasma Concentration - Time Curve Over the Dosing Interval (AUC[Tau]) - Part B	Pre-dose Day 1 and Day 28	AUC(tau) was defined as the area under the plasma concentration - time curve over the dosing interval.
Accumulation Index (AI): Part A and C	Baseline and Day 10	Accumulation index was calculated by dividing the AUC(tau) or Cmax or C24 of BMS-955176 on Day 10 by the AUC(TAU) or Cmax or C24, respectively, of BMS-955176 on Day 1.
Apparent Total Body Clearance: Part A and C	Baseline (Day 1) to Day 10	Apparent total body clearance was derived by non-compartmental methods, using a validated pharmacokinetic (PK) analysis program: KineticaTM 5.0 within eToolbox (version 2.7).
Degree of Fluctuation (DF): Part A and C	Baseline (Day 1) to Day 10	DF was calculated as the difference between Cmax and Cmin divided by Css-avg. DF was derived by non-compartmental methods, using a validated pharmacokinetic (PK) analysis program: KineticaTM 5.0 within eToolbox (version 2.7).
Average Observed Plasma Concentration at Steady State (Css-avg): Part A and C	Baseline (Day 1) to Day 10	Css-avg was calculated by the quotient of AUC(TAU) and the dosing interval (24 h). Css-avg was derived by non-compartmental methods, using a validated pharmacokinetic (PK) analysis program: KineticaTM 5.0 within eToolbox (version 2.7).
Plasma Half-life: Part A and C	Baseline (Day 1) to Day 10	Half-life of the terminal log-linear phase, (T-half), was calculated as natural logarithm of 2 (ln2)/λ, where λ is the absolute value of the slope of the terminal log-linear phase. T-half was derived by non-compartmental methods, using a validated pharmacokinetic (PK) analysis program: KineticaTM 5.0 within eToolbox (version 2.7).
Number of Participants With Clinically Significant Grade 3/4 Laboratory Abnormalities From Baseline	Day 1 to up to end of the study (Day 42)	Laboratory abnormalities were determined and graded using the Division of Acquired Immune Deficiency Syndrome (AIDS) Table for Grading the Severity of Adult and Pediatric Adverse Events, version 1.0, December 2004.
Number of Participants With Clinically Significant Changes in Heart Rate	Day 1 to end of the study (Day 42)	Heart rate was measured after the participants had been seated quietly for at least 5 minutes. Criteria used to determine heart rate that are outside of a pre-specified range, where changes from Baseline are based on matched postural positions and are calculated as parameter value - Baseline parameter value: Value \>100 and change from Baseline \> 30, or Value \< 55 and change from Baseline \< -15.
Number of Participants With Clinically Significant Changes in Electrocardiogram (ECG)	Day 1 to end of the study (Day 42)	Participants with out of range ECG intervals were summarized. Criteria used to determine ECG results that are outside of a pre-specified range: PR (milliseconds \[msec\]): Value \>200; QRS (msec): Value \>120; QT (msec): Value \>500 or change from Baseline \>30; corrected QT interval Fridericia's formula (QTcF) (msec): Value \>450 or change from Baseline \>30.
Number of Participants With Clinically Significant Changes in Systolic Blood Pressure (SBP) and Diastolic Blood Pressure (DBP)	Day 1 to end of the study (Day 42)	Systolic BP (millimeter of mercury \[mmHg\]): value \>140 and change from Baseline \>20, or value \<90 and change from Baseline \<-20; Diastolic BP (mmHg): value \>90 and change from Baseline \>10, or value \<55 and change from Baseline \<-10.
Number of Participants With Abnormal Changes in Physical Examination	Day 1 to end of the study (Day 42)	Participants with abnormal changes in physical examination is presented.