Mode
Text Size
Log in / Sign up
Phase 2 Completed N=50 Randomized Treatment

Pharmacodynamics, Safety and Pharmacokinetics of BMS-663068, an HIV Attachment Inhibitor, in HIV-1

Source: ClinicalTrials.gov NCT01009814 ↗
Enrolled (actual)
50
Serious AEs
0.0%
Results posted
Jan 2020
Primary outcomePrimary: Mean Logarithm With Base 10 (Log10) Change From Baseline in Human Immunodeficiency Virus (HIV) Ribonucleic Acid (RNA) at Day 9 — -1.3445; -1.2532; -1.2381; -1.1888 Log10 copies per milliliter (c/mL) — p=0.6102

Summary

Research Hypothesis: Administration of BMS-663068, a prodrug for HIV attachment inhibitor BMS-626529, will result in a mean decrease of at least 1 log10 in HIV RNA at Day 9 following 8 days of therapy in at least one dosing regimen that is safe and well tolerated in Clade B HIV-1 infected subjects.

Outcome Measures

OutcomeResultp-value
PRIMARY
Mean Logarithm With Base 10 (Log10) Change From Baseline in Human Immunodeficiency Virus (HIV) Ribonucleic Acid (RNA) at Day 9
-1.3445; -1.2532; -1.2381; -1.1888; -0.8760 0.6102
SECONDARY
Change From Baseline in Cluster of Differentiation 4 Positive (CD4+) Cell Count and Cluster of Differentiation 8 Positive (CD8+) Cell Count
114.2; 93.4; 109.8; 38.5; 32.0; 58.4
SECONDARY
Change From Baseline in Percent CD4+ Cell Count and Percent CD8+ Cell Count
-1.0; 1.2; 0.6; 0.1; 1.4; 1.6
SECONDARY
Number of Participants With Treatment Emergent Non-serious Adverse Event (Non-SAE) and Serious AE (SAE)
8; 5; 9; 8; 9; 0
SECONDARY
Number of Participants With Any Abnormality in Physical Examination
1; 0; 2; 1; 1
SECONDARY
Number of Participants With Worst-case Abnormalities in Diastolic Blood Pressure (DBP) and Systolic Blood Pressure (SBP)
0; 3; 1; 0; 1; 0
SECONDARY
Number of Participants With Worst-case Abnormalities in Body Temperature, Respiratory Rate [RR], and Heart Rate [HR]
0; 0; 0; 0; 0; 1
SECONDARY
Number of Participants With Worst-case Abnormalities in Electrocardiogram (ECG) Parameters
0; 1; 0; 0; 1; 0
SECONDARY
Number of Participants With Clinically Significant Abnormalities in Laboratory Parameters
0; 0; 0; 0; 0
SECONDARY
Maximum Observed Plasma Concentration (Cmax) of BMS-626529 Following Q12H Dosing
1.74; 3.52; 4.05; 2.55; 2.22; 5.55
SECONDARY
Cmax of BMS-626529 Following QHS Dosing
3.85; 3.47; 3.47
SECONDARY
Trough Observed Plasma Concentration (Ctrough) of BMS-626529 Following Q12H Dosing
0.349; 0.499; 0.640; 0.244; 0.473; 1.04
SECONDARY
Ctrough of BMS-626529 Following QHS Dosing
0.699; 0.0705; 0.0743; 0.0719; 0.0546; 0.0544
SECONDARY
Area Under the Concentration-time Curve in One Dosing Interval (AUC [Tau]) of BMS-626529 Following Q12H Dosing
9.16; 18.3; 20.6; 13.8; 13.1; 29.9
SECONDARY
AUC (Tau) of BMS-626529 Following QHS Dosing
25.5; 23.0
SECONDARY
Area Under the Concentration-time Curve Over a 24-hour Period (AUC [0-24]) of BMS-626529 Following Q12H Dosing
26.8; 60.6; 55.1; 42.6
SECONDARY
AUC (0-24) of BMS-626529 Following QHS Dosing
23.0
SECONDARY
Accumulation Index (AI) of BMS-626529 Following Q12H Dosing
1.53; 1.63; 1.34; 1.42
SECONDARY
Accumulation Index of BMS-626529 Following QHS Dosing
0.912
SECONDARY
Inhibitory Quotient (IQ) of BMS-626529 by Css,Avg and by Lowest Concentration of a Drug During Dosing Interval (Cmin) Following Q12H Dosing
11.0; 97.5; 67.2; 4.54; 29.7; 327
SECONDARY
Inhibitory Quotient (IQ) of BMS-626529 by Css,Avg and by Lowest Concentration of a Drug During Dosing Interval (Cmin) Following QHS Dosing
3.86; 67.8
SECONDARY
Inhibitory Quotient of BMS-626529 by Ctrough Following Q12H Dosing
12.2; 120; 87.3; 4.61
SECONDARY
Inhibitory Quotient of BMS-626529 by Ctrough Following QHS Dosing
4.77
SECONDARY
Cmax of Ritonavir Following Q12H Dosing
0.330; 0.314; 0.294; 1.31; 1.30; 0.841
SECONDARY
Cmax of Ritonavir Following QHS Dosing
0.257; 0.628; 0.628
SECONDARY
Ctrough of Ritonavir Following Q12H Dosing
0.117; 0.131; 0.502; 0.554; 0.0831; 0.526
SECONDARY
Ctrough of Ritonavir Following QHS Dosing
0.157; 0.107; 0.0845; 0.0844; 0.0808; 0.0830
SECONDARY
AUC (Tau) of Ritonavir Following Q12H Dosing
2.37; 2.05; 9.43; 9.05; 6.76; 9.23
SECONDARY
AUC (Tau) of Ritonavir Following QHS Dosing
2.91; 6.13
SECONDARY
AUC (0-24) of Ritonavir Following Q12H Dosing
18.9; 19.5; 6.76
SECONDARY
AUC (0-24) of Ritonavir Following QHS Dosing
6.13
SECONDARY
Accumulation Index of Ritonavir Following Q12H Dosing
3.58; 4.41; 3.62
SECONDARY
Accumulation Index of Ritonavir Following QHS Dosing
2.19

Eligibility Criteria

Inclusion Criteria

  • Clade B HIV-1 infected subjects meeting following criteria at screening:
  • Plasma HIV RNA ≥ 5,000 copies/mL
  • CD4+ lymphocyte ≥ 200 cells/µL
  • Antiretroviral naive or experienced
  • Off all ARV therapy with HIV activity for > 8 weeks
  • BMI of 18 to 35 kg/m2, inclusive.
  • Not currently co-infected with HCV or HBV
  • Men and women, ≥ 18 years of age

Exclusion Criteria

  • Woman of childbearing potential (WOCBP) unwilling or unable to use an acceptable method to avoid pregnancy for the entire study period up to 12 weeks after the last dose of study drug.
  • WOCBP using prohibited contraceptive method including oral, injectable, or implantable hormonal contraceptive agent within 12 weeks of enrollment.
  • Women who are pregnant or breastfeeding.
  • Women with positive pregnancy test on enrollment or prior to study drug intake.
  • Sexually active fertile men not using effective birth control during study and for at least 12 weeks after last dose of study drug if partners are WOCBP.
  • Significant acute or chronic medical illness not stable or not controlled with medication or not consistent with HIV infection.
  • Current or recent (within 3 months) gastrointestinal disease that, in the opinion of Investigator or Medical Monitor, may impact on drug absorption and/or put subject at risk for GI tract irritation and/or bleeding.
  • Acute diarrhea lasting ≥ 1 day, within 3 weeks prior to randomization.
  • Major surgery within 4 weeks of study drug intake.
  • Gastrointestinal surgery that could impact upon absorption of study drug.
  • Donation of blood or plasma to blood bank or in a clinical study (except a Screening visit or follow up visit of less than 50 mL) within 4 weeks of study drug intake.
  • Blood transfusion within 4 weeks of study drug intake.
  • Inability to tolerate oral medication.
  • Inability to be venipunctured and/or tolerate venous access.
  • Personal history of clinically relevant cardiac disease, symptomatic or asymptomatic arrhythmias, syncopal episodes, or additional risk factors for torsades de pointes.
  • Personal or family history of long QT syndrome.
  • Recent (within 6 months) drug/alcohol abuse
  • Any other medical, psychiatric and/or social reason which, in the opinion of the Investigator, would make the candidate inappropriate for participation.
  • Evidence of organ dysfunction or clinically significant deviation from normal in physical examination, vital signs, ECG or clinical lab determinations or not consistent with subject's degree of HIV infection.
  • Evidence of 2nd or 3rd degree heart block at screening or Day -1
  • Positive urine drug screen at Screening or Day -1 without valid prescription (subjects positive for cannabinoids and/or amphetamines will be included).
  • Positive blood screen for hepatitis B surface antigen.
  • Positive blood screen for hepatitis C antibody and hepatitis C RNA.
  • History of significant drug allergy
  • Exposure to any investigational drug or placebo within 4 weeks of study drug intake.
  • Prescription drugs within 4 weeks prior to study drug intake, unless approved by BMS medical monitor.
  • Other drugs, including over-the-counter medications, vitamins and/or herbal preparations, within 1 week prior to study drug intake, unless approved by BMS medical monitor.
  • Use of oral, injectable or implantable hormonal contraceptive agent within 12 weeks of study drug intake.
  • Use of prescription drugs or OTC drugs that may cause GI tract irritation or bleeding within 2 weeks of study drug intake, unless approved by BMS medical monitor.
  • Use of alcohol-containing beverages within 3 days prior to study drug intake.
  • Use of grapefruit, grapefruit-containing or Seville orange-containing products within 7 days prior to study drug intake.
  • Prisoners or subjects involuntarily incarcerated.
  • Subjects compulsorily detained for treatment of either a psychiatric or physical illness.
View full record on ClinicalTrials.gov →

Data sourced from ClinicalTrials.gov (NCT01009814). Outcome figures and adverse-event rates are extracted automatically from the registry's posted results and are provided for clinician reference, not as a substitute for the primary publication. Informational only — not medical advice.

Back to search