CCR5 Inhibitor Treatment Intensification on CD4+ T-cell Recovery
Study Details
Study Description
Brief Summary
CCTG 590 is a open-label study to evaluate the impact of therapy intensification with Maraviroc (MVC) (a CCR5 inhibitor) to a stable suppressive HIV antiretroviral regimen on the rate of CD4+ T-cell recovery and gene expression profiles. Patients on a stable first-line HIV regimen with continued viral suppression and sub-optimal CD4+ T-cell counts will be eligible for this study. Those who are found to be eligible will have MVC (dose-adjusted to background HIV regimen) added to their current HIV regimen for 24 weeks. After the 24 week intensification, the MVC will be discontinued, the original antiretroviral regimen will be continued and the subjects will be followed for an additional 12 weeks.
The investigators hypothesize that MVC will improve the rate of CD4 recovery. This improved CD4 recovery will be associated with favorable changes in gene expression profiles of genes involved with CD4 maintenance and circulation.
Condition or Disease | Intervention/Treatment | Phase |
---|---|---|
Phase 4 |
Detailed Description
Blunted CD4+ T-cell responses during viral control may be a consequence of on-going T-cell destruction in the regenerative phase of CD4 recovery from activation-induced apoptosis and/or reduced production from decreased thymic output. Maraviroc, a CCR5 inhibitor, may improve the clinical status of HIV-infected by two distinct mechanisms. First, by blocking HIV entry into CD4+ T-cells, CCR5 inhibitors have direct antiviral activity. Second, as the pro-inflammatory state of HIV infection up-regulates CCR5 ligands and receptors, this CCR5 receptor antagonist may abrogate immune activation and resultant T-cell apoptosis. Importantly, MVC binds CCR5 receptors without inducing intracellular signaling or altering cell-surface expression. Potentially, MVC intensification during viral suppression with ART may further decrease persistent activation-induced apoptosis and improve repair and remodeling of lymphoid tissue leading to increased CD4+ T-cell recovery and function.
The aim of this study is to evaluate a potentially therapeutic immunomodulatory effect of MVC. Several measures of immune homeostasis will be determined in this study, including functional genomic analysis and extended T-cell phenotyping. Genes responsive to MVC therapy will be identified and categorized into functional groups. Based upon existing literature of the identified genes and observed immune responses (change in CD4/CD8 subsets) during MVC therapy, a model of CCR5 responsive-genes and potential impact on immune recovery will be outlined. Potentially, individuals experiencing immune discordance during suppressive ART may be better treated by MVC antiretroviral intensification.
-
We hypothesize that expression will decrease among genes involved in immune activation (NF-kB, MAPK, nuclear factor of activated T-cells, MYD88 and STAT1), apoptosis (Fas ligand and TRAIL) and trafficking/repopulation of T-cells (CCR5, MIP-1α, MIP-1β and RANTES) and increase among genes involved in tissue repair (platelet-derived growth factor, insulin-like growth proteins and osteoblast-specific transcription factor).
-
The gene expression profiles induced by MVC will be associated with a favorable increase in the rate of CD4+ T-cell recovery.
-
The rate of CD4 recovery (cells/month) will be greater during MVC compared to before.
-
The proportion of cells expressing activation/ apoptosis markers will decrease from baseline and this decrease will be associated with improved CD4 recovery.
-
The proportion of naïve cells will increase from baseline and this increase will be associated with improved CD4 recovery.
-
The rate of CD4 recovery will be greater among those subjects receiving PI-containing treatment regimens compared to those receiving NNRTI-containing treatment regimen.
Study Design
Arms and Interventions
Arm | Intervention/Treatment |
---|---|
Experimental: Maraviroc 150 mg, 300 mg, or 600 mg twice daily This was a single arm study where Maraviroc was added for 24 weeks. Maraviroc was dose-adjusted for concomitantly administered HIV medications according to the manufacture's recommendations: 150 mg twice daily with strong CYP3A4 inhibitors, including: Protease inhibitors (except tipranavir/ ritonavir) Delavirdine ketoconazole, itraconazole, clarithromycin, nefazadone, telithromycin Darunavir/r + etravirine 300 mg twice daily with non-inducers/ non-inhibitors of CYP3A4, including: Tipranavir/ ritonavir Nevirapine All NRTIs Enfuvirtide 600 mg twice daily with strong CYP3A4 inducers, including: Efavirenz, etravirine rifampin |
Drug: Maraviroc
Maraviroc will be given dose-adjusted to background HIV treatment (150 mg, 300 mg, or 600 mg twice daily)
Other Names:
|
Outcome Measures
Primary Outcome Measures
- Differences in Gene Expression Profiles Obtained at Baseline and Week 4 and Week 24. [Baseline to Week 24]
To determine differential gene expression in T-Cells due to MVC exposure between week 0, 4 and 24 weeks. Repeated measures (RM) ANOVA was used to identify genes whose expression changed over the course of MVC administration. Multivariate permutation tests under default settings (80% confident no more than 10% false positives) were performed using BRB-Array Tools. Gene assignment to temporal profiles was performed using a non- parametric clustering algorithm in Short Time-series Expression Miner (STEM)
Secondary Outcome Measures
- CD4+ T-cell Absolute Count and Percentage at Baseline, Weeks 4 and 24. [Baseline to Week 24]
To compare the CD4+/CD8+ T-cell absolute count and percentage change at Weeks 4 and 24 from Baseline. Wilcoxon signed rank test was used to assess changes in T cell counts, percentages, CD4+ T cell recovery slopes and changes in T cell phenotypes measured by flow cytometry.
- Change in CD4+/CD8+ T-cell Immune Activation, Maturation, Regulatory and Apoptosis Markers at Baseline and Weeks 4 and 24. [Baseline to Week 24]
To compare the percent change of CD4+/CD8+ T-cell
Eligibility Criteria
Criteria
Inclusion Criteria:
-
HIV-1 infection
-
All available CD4+ T cell counts within the last 12 months of screening below 350 cells/mm3 (minimum of 3 values obtained > 30 days apart).
-
HIV treatment with a stable (for at least 6 months) antiretroviral regimen consisting of at least 2 NRTIs and either a protease inhibitor boosted with low dose ritonavir or an NNRTI. A stable regimen is defined as no additions or deletions for more than 14 cumulative days.
-
Patient considered to be receiving initial HIV regimen (history of medication substitution for toxicity is allowed).
-
All available plasma HIV RNA levels within the last 12 months are below the level of detection. Isolated values that are detectable but < 1000 copies will be allowed as long as the plasma HIV RNA levels before and after this detectable time point are undetectable - The subject should have a minimum of 3 values obtained > 30 days apart.
-
Females of childbearing potential must have a negative serum pregnancy test at screening and agree to use a double-barrier method of contraception throughout the study period.
-
Men and women age ≥ 18 years.
Exclusion Criteria:
-
Current antiretroviral regimen contains tenofovir disoproxil fumarate AND didanosine in combination.
-
History of chronic hepatitis C (defined as HCV antibody positive and HCV RNA detectable).
-
History of chronic active hepatitis B (defined as surface antibody negative, surface antigen positive and HBV DNA detectable).
-
Concurrent use of G-CSF or GM-CSF.
-
Prior or concurrent use of IL-2.
-
Prior or concurrent use of a CCR5 inhibitor.
-
Active drug or alcohol use or dependence that, in the opinion of the investigator, would interfere with adherence to study requirements.
-
Use of any immunomodulator, HIV vaccine, or investigational therapy within 30 days of study entry.
-
Use of human growth hormone within 30 days prior to study entry.
-
Initiation of testosterone or anabolic steroids within 30 days prior to study entry. (Exception: Chronic replacement dosages in patient's with diagnosed hypogonadism is allowed).
-
Evidence of splenic sequestration or suppressed bone marrow function:
-
Clinical or radiographic evidence of significant splenomegaly.
-
History of leukemia or lymphoma.
-
History of myelosuppressive chemotherapy or irradiation
Contacts and Locations
Locations
Site | City | State | Country | Postal Code | |
---|---|---|---|---|---|
1 | University Southern California | Los Angeles | California | United States | 90033 |
2 | University California San Diego | San Diego | California | United States | 92103 |
3 | Harbor-UCLA | Torrance | California | United States | 90502 |
Sponsors and Collaborators
- University of California, San Diego
- University of California, Los Angeles
- University of Southern California
- Pfizer
- California HIV/AIDS Research Program
Investigators
- Study Chair: Sheldon Morris, MD, UC San Diego AntiViral Research Center (AVRC)
- Principal Investigator: Richard Haubrich, MD, University of California, San Diego
Study Documents (Full-Text)
More Information
Publications
None provided.- CCTG 590
Study Results
Participant Flow
Recruitment Details | |
---|---|
Pre-assignment Detail |
Arm/Group Title | Maraviroc Intensification |
---|---|
Arm/Group Description | Maraviroc will be added to patient's existing HIV treatment regimen dose-adjusted to background HIV medications Maraviroc: Maraviroc will be given dose-adjusted to background HIV treatment |
Period Title: Overall Study | |
STARTED | 32 |
COMPLETED | 32 |
NOT COMPLETED | 0 |
Baseline Characteristics
Arm/Group Title | Maraviroc Intensification |
---|---|
Arm/Group Description | Maraviroc will be added to patient's existing HIV treatment regimen dose-adjusted to background HIV medications Maraviroc: Maraviroc will be given dose-adjusted to background HIV treatment |
Overall Participants | 32 |
Age (years) [Mean (Standard Deviation) ] | |
Mean (Standard Deviation) [years] |
48.9
(9.7)
|
Sex: Female, Male (Count of Participants) | |
Female |
4
12.5%
|
Male |
28
87.5%
|
Race/Ethnicity, Customized (Count of Participants) | |
White, not Hispanic |
7
21.9%
|
Black |
2
6.3%
|
White Hispanic |
21
65.6%
|
Other |
2
6.3%
|
Outcome Measures
Title | Differences in Gene Expression Profiles Obtained at Baseline and Week 4 and Week 24. |
---|---|
Description | To determine differential gene expression in T-Cells due to MVC exposure between week 0, 4 and 24 weeks. Repeated measures (RM) ANOVA was used to identify genes whose expression changed over the course of MVC administration. Multivariate permutation tests under default settings (80% confident no more than 10% false positives) were performed using BRB-Array Tools. Gene assignment to temporal profiles was performed using a non- parametric clustering algorithm in Short Time-series Expression Miner (STEM) |
Time Frame | Baseline to Week 24 |
Outcome Measure Data
Analysis Population Description |
---|
32 participants received intervention and were followed for CD4+ counts. 25 of 32 participants had microarray analysis done. |
Arm/Group Title | Maraviroc Intensification |
---|---|
Arm/Group Description | Maraviroc will be added to patient's existing HIV treatment regimen dose-adjusted to background HIV medications Maraviroc: Maraviroc will be given dose-adjusted to background HIV treatment |
Measure Participants | 25 |
Number [-fold TNF downregulation] |
1.44
|
Title | CD4+ T-cell Absolute Count and Percentage at Baseline, Weeks 4 and 24. |
---|---|
Description | To compare the CD4+/CD8+ T-cell absolute count and percentage change at Weeks 4 and 24 from Baseline. Wilcoxon signed rank test was used to assess changes in T cell counts, percentages, CD4+ T cell recovery slopes and changes in T cell phenotypes measured by flow cytometry. |
Time Frame | Baseline to Week 24 |
Outcome Measure Data
Analysis Population Description |
---|
[Not Specified] |
Arm/Group Title | Maraviroc Intensification |
---|---|
Arm/Group Description | Maraviroc will be added to patient's existing HIV treatment regimen dose-adjusted to background HIV medications Maraviroc: Maraviroc will be given dose-adjusted to background HIV treatment |
Measure Participants | 32 |
Wk 4 CD4+ cells (absolute) |
6.50
|
Wk 4 CD8+ cells (absolute) |
46
|
Wk 24 CD4+ cells (absolute) |
36.75
|
Wk 24 CD8+ cells (absolute) |
100.00
|
Title | Change in CD4+/CD8+ T-cell Immune Activation, Maturation, Regulatory and Apoptosis Markers at Baseline and Weeks 4 and 24. |
---|---|
Description | To compare the percent change of CD4+/CD8+ T-cell |
Time Frame | Baseline to Week 24 |
Outcome Measure Data
Analysis Population Description |
---|
[Not Specified] |
Arm/Group Title | Maraviroc Intensification |
---|---|
Arm/Group Description | Maraviroc will be added to patient's existing HIV treatment regimen dose-adjusted to background HIV medications Maraviroc: Maraviroc will be given dose-adjusted to background HIV treatment |
Measure Participants | 32 |
Wk 4 CD4+ total |
0.62
|
Wk 4 CD4+ naive |
-0.47
|
Wk 4 CD4+ central memory |
0.43
|
Wk 4 CD4+ effector memory |
-0.33
|
Wk 4 CD4+ effector |
0.00
|
Wk 4 CD4+ immune senescence |
-0.12
|
Wk 24 CD4+ total |
1.12
|
Wk 24 CD4+ naive |
0.52
|
Wk 24 CD4+ central memory |
-0.15
|
Wk 24 CD4+ effector memory |
-0.30
|
Wk 24 CD4+ effector |
0.00
|
Wk 24 CD4+ immune senescence |
-0.25
|
Wk 4 CD8+ total |
0.90
|
Wk 4 CD8+ naive |
-0.45
|
Wk 4 CD8+ central memory |
0.83
|
Wk 4 CD8+ effector memory |
0.73
|
Wk 4 CD8+ effector |
-0.90
|
Wk 4 CD8+ immune senescence |
-1.83
|
Wk 24 CD8+ total |
2.38
|
Wk 24 CD8+ naive |
-0.15
|
Wk 24 CD8+ central memory |
0.75
|
Wk 24 CD8+ effector memory |
0.80
|
Wk 24 CD8+ effector |
-2.68
|
Wk 24 CD8+ immune senescence |
-3.30
|
Adverse Events
Time Frame | ||
---|---|---|
Adverse Event Reporting Description | ||
Arm/Group Title | Maraviroc Intensification | |
Arm/Group Description | Maraviroc will be added to patient's existing HIV treatment regimen dose-adjusted to background HIV medications Maraviroc: Maraviroc will be given dose-adjusted to background HIV treatment | |
All Cause Mortality |
||
Maraviroc Intensification | ||
Affected / at Risk (%) | # Events | |
Total | 0/32 (0%) | |
Serious Adverse Events |
||
Maraviroc Intensification | ||
Affected / at Risk (%) | # Events | |
Total | 1/32 (3.1%) | |
Psychiatric disorders | ||
Altered mental status | 1/32 (3.1%) | 1 |
Other (Not Including Serious) Adverse Events |
||
Maraviroc Intensification | ||
Affected / at Risk (%) | # Events | |
Total | 0/32 (0%) |
Limitations/Caveats
More Information
Certain Agreements
Principal Investigators are NOT employed by the organization sponsoring the study.
There is NOT an agreement between Principal Investigators and the Sponsor (or its agents) that restricts the PI's rights to discuss or publish trial results after the trial is completed.
Results Point of Contact
Name/Title | Sheldon Morris |
---|---|
Organization | UCSD |
Phone | 6195438080 |
shmorris@ucsd.edu |
- CCTG 590